C-Reactive Protein as a Risk Factor for Coronary Heart Disease: A Systematic Review and Meta-analyses for the U.S. Preventive Services Task Force

doi:10.1059/0003-4819-151-7-200910060-00009

C-Reactive Protein as a Risk Factor for Coronary Heart Disease: A Systematic Review and Meta-analyses for the U.S. Preventive Services Task Force

David I. Buckley, MD, MPH;
Rongwei Fu, PhD;
Michele Freeman, MPH;
Kevin Rogers, MD; and
Mark Helfand, MD, MPH

From the Oregon Evidence-based Practice Center, Oregon Health & Science University, and Veterans Affairs Medical Center, Portland, Oregon, and University of Utah Health Sciences Center, Salt Lake City, Utah.

Abstract

Background: C-reactive protein (CRP) may help to refine global risk assessment for coronary heart disease (CHD), particularly among persons who are at intermediate risk on the basis of traditional risk factors alone.

Purpose: To assist the U.S. Preventive Services Task Force (USPSTF) in determining whether CRP should be incorporated into guidelines for CHD risk assessment.

Data Sources: MEDLINE search of English-language articles (1966 to November 2007), supplemented by reference lists of reviews, pertinent studies, editorials, and Web sites and by expert suggestions.

Study Selection: Prospective cohort, case–cohort, and nested case–control studies relevant to the independent predictive ability of CRP when used in intermediate-risk persons.

Data Extraction: Included studies were reviewed according to predefined criteria, and the quality of each study was rated.

Data Synthesis: The validity of the body of evidence and the net benefit or harm of using CRP for CHD risk assessment were evaluated. The combined magnitude of effect was determined by meta-analysis. The body of evidence is of good quality, consistency, and applicability. For good studies that adjusted for all Framingham risk variables, the summary estimate of relative risk for incident CHD was 1.58 (95% CI, 1.37 to 1.83) for CRP levels greater than 3.0 mg/L compared with levels less than 1.0 mg/L. Analyses from 4 large cohorts were consistent in finding evidence that including CRP improves risk stratification among initially intermediate-risk persons. C-reactive protein has desirable test characteristics, and good data exist on the prevalence of elevated CRP levels in intermediate-risk persons. Limited evidence links changes in CRP level to primary prevention of CHD events.

Limitations: Study methods for measuring Framingham risk variables and other covariates varied. Ethnic and racial minority populations were poorly represented in most studies, limiting generalizability. Few studies directly assessed the effect of CRP on risk reclassification in intermediate-risk persons.

Conclusion: Strong evidence indicates that CRP is associated with CHD events. Moderate, consistent evidence suggests that adding CRP to risk prediction models among initially intermediate-risk persons improves risk stratification. However, sufficient evidence that reducing CRP levels prevents CHD events is lacking.

In the United States, cardiovascular disease accounts for nearly 40% of all deaths each year (1). The factors that make up the Framingham risk score (age, sex, blood pressure, serum total cholesterol or low-density lipoprotein cholesterol level, high-density lipoprotein cholesterol level, cigarette smoking, and diabetes) account for most of the excess risk for incident coronary heart disease (CHD) (2, 3). However, these factors do not explain all of the excess risk (4, 5), and approximately 40% of CHD deaths occur in persons with cholesterol levels that are lower than the population average (6). Several lines of evidence (7, 8) have implicated chronic inflammation in CHD, and inflammatory markers have received much attention as new or emerging risk factors that could account for some of the unexplained variability in CHD risk.

C-reactive protein (CRP) is a sensitive, nonspecific systemic marker of inflammation (9). Although it is unknown whether CRP is involved in CHD pathogenesis (10, 11), elevated serum CRP levels are associated with traditional cardiovascular risk factors and obesity (12, 13). In 2002, an expert panel recommended against routine use of CRP in risk assessment for primary prevention of CHD but supported CRP measurement in persons with a 10-year CHD risk of 10% to 20%. It noted that the benefits of this strategy “remain uncertain” and recommended further research into the implications of using CRP in risk categorization for therapeutic risk reduction in patients (14).

The potential clinical benefit of new risk factors for refining global risk assessment is thought to be greatest for persons who are classified as intermediate-risk when stratified by using conventional risk factors (15). In the Framingham risk scoring system, intermediate-risk persons are those with a 10% to 20% risk for coronary death or nonfatal myocardial infarction (“hard CHD events”) over 10 years. Further stratification by using new markers might reclassify some intermediate-risk persons as low-risk (10-year risk <10%) and others as high-risk (10-year risk >20%). This would permit more aggressive risk reduction therapy in persons reclassified as high-risk and may consequently reduce incident CHD events (16).

Several previous meta-analyses (17–19) have assessed the possible independent predictive ability of CRP level for incident CHD risk. In 1998, a meta-analysis of 5 long-term, population-based prospective cohort studies and 2 cohorts of patients with preexisting CHD (17) calculated a risk ratio for coronary events of 1.7 (95% CI, 1.4 to 2.1) for CRP levels in the top tertile versus the bottom tertile. An update of this meta-analysis in 2000 (18) included 7 additional studies. The combined risk ratio for the 11 population-based prospective cohort studies of persons without preexisting CHD was 2.0 (CI, 1.6 to 2.5). Another update in 2004 (19) included 11 new studies as well as the 11 previous cohorts. The combined odds ratio for all 22 studies was 1.58 (CI, 1.48 to 1.69).

These 3 meta-analyses, however, lacked a systematic assessment of the characteristics and quality of study design and execution. In particular, they did not systematically assess the degree of adjustment for standard measures of CHD risk (such as the Framingham risk score). Although the first 2 meta-analyses reported the degree of adjustment for potential confounders in each of the included studies, they did not specify how many or which standard coronary risk factors were adjusted for. Furthermore, these meta-analyses did not use the degree of adjustment as a basis for quality rating or inclusion. The most recent meta-analysis (19) did not rate quality or degree of adjustment for potential confounders. In addition, because the investigators used broad inclusion criteria, the studies in these meta-analyses do not necessarily represent the intermediate-risk population.

We conducted a systematic review and meta-analyses of epidemiologic studies to help the U.S. Preventive Services Task Force (USPSTF) determine whether CRP level should be incorporated into guidelines for coronary and cardiovascular risk assessment in primary care. Our review addresses the question of whether elevated CRP levels are independently predictive of incident CHD events, specifically among intermediate-risk persons. Our approach incorporated elements previously used by the USPSTF (20) and several domains of the approach developed by the Grading of Recommendations, Assessment, Development, and Evaluation workgroup (21).

Previous Section Next Section

Methods

Data Sources and Searches

We searched MEDLINE for original epidemiologic studies published between 1966 and November 2007. Our search strategy included the terms cardiovascular diseases, C-reactive protein, inflammation, and biological markers and was limited to articles published in English. We obtained additional articles from recent systematic reviews; reference lists of pertinent studies, reviews, editorials, and Web sites; and consultations with experts.

Study Selection

We included studies that published original data relevant to measuring the increased risk for incident CHD associated with elevated CRP level. We only considered prospective cohort studies (including those based on a cohort within a randomized trial), case–cohort studies, and nested case–control studies. We only included studies that had a follow-up of 2 years or more, reported the outcomes of coronary death and nonfatal myocardial infarction, and adjusted for a minimum of 5 of the 7 risk factors used in the Framingham risk score. We excluded studies in which no participants were likely to be classified as intermediate-risk by using the Framingham risk score and those conducted exclusively in patients with previously diagnosed coronary disease, coronary disease equivalents (such as diabetes), or medical conditions that may cause premature CHD. We included studies in which some patients had cardiovascular disease at baseline only if the studies adjusted for prevalent disease in their analysis. The full systematic evidence report (22) provides a more detailed description of our study methods.

Data Extraction and Quality Assessment

One investigator reviewed the relevant articles and recorded overlap with the studies included in previous meta-analyses. For our meta-analyses, when multiple articles were published from a single cohort, we included the findings from the analysis with the highest applicability to the study question and the highest validity, on the basis of our quality ratings. In general, we selected cohort studies over nested case–control studies, good-quality studies over fair-quality studies, studies that adjusted for more Framingham risk variables, studies with longer follow-up, and studies that most closely addressed our principal question.

We used standardized forms to abstract data on study design, population, size, CRP measurement, Framingham risk factor measurement, length of follow-up, outcomes, and data analysis. For each study, we recorded how many Framingham risk factors and other confounding factors were included in the model; whether the investigators reported model fit measures, discrimination measures, or model calibration statistics separately for models with and without CRP; and whether the study assessed the degree to which persons were reclassified on the basis of CRP level, overall or in the intermediate-risk group.

Two investigators used the USPSTF criteria (20) to independently assess the quality of each study as good, fair, or poor. These criteria are specific to the study design (cohort or nested case–control) and include such items as appropriate assembly or ascertainment of the cohort or the case patients and control participants, reliability and equal application of measurements, response or follow-up rate, and appropriate adjustment for confounding. Because we sought to evaluate the predictive ability of CRP independent of the Framingham risk factors, we required that a study adjust for all 7 of the Framingham variables to receive a quality rating of “good,” even if the study otherwise had high internal validity. We resolved disagreements regarding quality by discussion, further review, and adjudication by a third reviewer (if necessary).

Data Synthesis and Analysis

The ideal approach to assessing the clinical effect of expanding the Framingham risk score has been debated extensively. Most previous research on the effect of a new risk factor has focused on the c-statistic, a measure of discrimination. The c-statistic, however, may be a poor indicator of the effect of using CRP level to further stratify persons classified as intermediate-risk by the Framingham risk score. For this reason, recent literature (23–26) has emphasized that studies should examine how well assessing CRP level improves risk prediction and further risk stratification among persons initially classified as intermediate-risk.

Most studies provided an overall estimate of the risk associated with high CRP levels, after adjustment for other risk factors, but did not provide specific evidence about the intermediate-risk group. For these studies, we conducted 2 meta-analyses to obtain pooled adjusted risk ratios for the association of hard CHD events and CRP level. The first included all studies that were fair-quality or better, adjusted for at least 5 Framingham risk factors, included at least some participants who were likely to be at intermediate risk, and estimated the risk for CHD associated with CRP level after adjusting for confounders. Because including studies that had methodological flaws or assessed fewer Framingham risk factors could have led to overestimation of the pooled risk ratio, we conducted a second meta-analysis that was restricted to good-quality studies, all of which adjusted for all Framingham risk factors.

Because different studies reported ratios for different cutoff levels (including tertiles, quartiles, or quintiles), or as an increase in risk for a given unit of increase in CRP level, we standardized the risk ratio of CRP level for our meta-analyses to provide clinically relevant and easily interpretable results. We used currently recommended cutoff points (14) for low (<1.0 mg/L), average (1.0 to 3.0 mg/L), and high (>3.0 mg/L), with less than 1.0 mg/L as a reference. When studies used other cutoff points to categorize CRP level, we calculated risk ratios at cutoff points of 1.0 and 3.0 mg/L by assuming a log-normal distribution of CRP level (17, 27) and a log-linear association of CHD risk over the midrange of log-CRP levels (17, 28). We estimated distribution parameters of CRP level from published information from each study. We estimated CIs by using reported SEs for the coefficient of CRP level when studies analyzed CRP level as a continuous variable and by applying the same assumption of a log-linear relationship when studies categorized CRP level by using other cutoff points. We combined the risk ratio estimates by using a random-effects model to incorporate variation among studies into the combined estimate (29). We assessed statistical heterogeneity among the studies by using standard chi-square tests and estimated the magnitude of heterogeneity by using the I² statistic (30). We used random-effect meta-regression to examine possible sources of heterogeneity and investigate whether the risk ratio estimates were associated with various study-level characteristics (30). We tested whether the distribution of the effect sizes was symmetric with respect to the precision measure by using funnel plots and the Egger linear regression method (31). We used Stata, version 10.0 (StataCorp, College Station, Texas), to perform the analyses.

Although our meta-analyses addressed whether CRP adds information to the Framingham risk score, they could not assess how well risk ratios derived from the entire population apply to intermediate-risk participants, or how those participants would be reclassified if CRP were used. To examine reclassification, we identified and critically appraised the studies that either compared predictive models that used all Framingham risk factors, with and without CRP levels, or measured the incidence of CHD events among intermediate-risk participants classified by CRP levels.

Role of the Funding Source

The Agency for Healthcare Research and Quality suggested the topic and provided copyright release for this manuscript but did not participate in the literature search, data analysis, or interpretation of the results.

Previous Section Next Section

Results

Study Characteristics

Of 1292 abstracts of potentially relevant studies, 37 published studies (8, 18, 19, 23, 28, 32–63) conducted in 24 cohorts met our inclusion criteria (Appendix Figure). (Appendix Tables 1 and 2, have more information on these studies.) From these, we identified 23 principal articles that represented the most pertinent publication for meta-analysis from each of the 24 cohorts (18, 19, 28, 33, 35, 37, 42–46, 48, 50–52, 54–56, 59–63) (Table). All but 1 study (37) explicitly excluded patients with baseline CHD or cardiovascular disease, and this study adjusted for prevalent CHD. All studies measured CRP level by using a high-sensitivity CRP assay.

View larger version:

Appendix Figure. Literature search and selection.

FRS = Framingham risk score.

View this table:

Table. Study Characteristics and Adjusted Estimates of CHD Risk Associated With CRP

Thirteen of the 24 cohorts in our review were also included in the 2004 meta-analysis (19). Five of these 13 cohorts were represented by the same article in both our meta-analysis and the previous meta-analysis (18, 19, 46, 48, 54). For the other 8, we used more recent articles (33, 37, 42, 51, 52, 56, 59, 60). We included 1 additional cohort study published in 2002 (28) and studies from 10 new cohorts published after the timeframe of the previous meta-analysis (35, 43–45, 50, 55, 61–63). We excluded studies from 8 cohorts that the previous meta-analysis had included. Most of these were studies in which the participants were or were likely to be at increased risk for CHD (64–69). We excluded 2 studies from our review because they studied mortality only (70, 71). We rated 10 studies in 11 of the 24 cohorts as good-quality (33, 42, 44–46, 52, 55, 56, 60, 61) and 13 studies in 14 cohorts as fair-quality (18, 19, 28, 35, 37, 43, 48, 50, 51, 54, 59, 62, 63). Baseline CRP level was positively associated with incident CHD events in 23 of the 24 cohorts, with adjusted relative risks that ranged from 0.98 to 2.61.

Meta-analysis of Fair-Quality or Better Studies

Our meta-analysis of the 22 studies (in 23 cohorts) that explicitly excluded baseline CHD yielded a risk ratio of 1.60 (CI, 1.43 to 1.78) for high versus low CRP levels (Figure 1) and 1.26 (CI, 1.17 to 1.35) for average versus low CRP levels (Figure 2). Including the study that did not explicitly exclude baseline CHD (37) did not appreciably change the combined risk ratio estimates. We found statistically significant heterogeneity of effects among studies at a P value less than 0.100, both for the comparison of high versus low CRP levels (I² = 31.9%; P = 0.072) and average versus low CRP levels (I² = 44.0%; P = 0.015). However, the standardized estimates of effect were consistently positive, with a range of 0.98 to 2.75 for high CRP levels and 0.99 to 1.88 for average CRP levels. Furthermore, the positive relationship persisted in analyses of all subgroups at both high and average levels of CRP (Figure 3). In subgroup meta-regression analyses, we found no statistically significant differences among categories for any study-level characteristic, including number of Framingham variables and other covariates adjusted, outcome measures (major CHD events vs. major CHD plus other CHD events or cardiovascular events), study design, sex, quality rating, and length of follow-up. We conducted a sensitivity analysis to compare the 17 studies that required standardization of risk ratios with the 6 studies that used recommended cutoffs. The combined risk ratio estimates were similar between the 2 groups of studies. We detected no statistically significant asymmetry when we examined funnel plots or used the Egger linear regression method and no evidence of a tendency for smaller studies to show a larger degree of association.

View larger version:

Figure 1. Risk ratio for coronary heart disease associated with C-reactive protein level >3.0 versus <1.0 mg/L.

* Number of participants included in the analysis.

View larger version:

Figure 2. Risk ratio for coronary heart disease associated with C-reactive protein level 1.0 to 3.0 versus <1.0 mg/L.

View larger version:

Figure 3. Analyses of all subgroups at high (>3.0 mg/L) and average (1.0 to 3.0 mg/L) CRP levels.

CHD = coronary heart disease; CRP = C-reactive protein; CVD = cardiovascular disease.

* Number of cohorts included in the analysis.

† Framingham risk factors are based on reference 2.

Meta-analysis of Good-Quality Studies

We also performed a meta-analysis limited to the 10 good-quality studies from 11 cohorts, all of which adjusted for all Framingham risk factors or calculated a Framingham risk score (33, 42, 44–46, 52, 55, 56, 60, 61). The relative risk was 1.58 (CI, 1.37 to 1.83) for high versus low CRP levels (Figure 1) and 1.22 (CI, 1.11 to 1.33) for average versus low CRP levels (Figure 2). We found no statistically significant heterogeneity of effects among studies in this analysis. We excluded 4 fair-quality studies that used all Framingham risk factors (43, 50, 59, 62). We conducted a sensitivity analysis and found similar results with and without these 4 studies. The relative risk was 1.53 (CI, 1.36 to 1.73) for high versus low CRP levels and 1.20 (CI, 1.12 to 1.29) for average versus low CRP levels.

Reclassification of Persons at Intermediate Risk

From a clinical perspective, the most meaningful measure of CRP's value as a marker is its effect on rates of reclassification from intermediate-risk to other risk categories. Recent articles (24–26, 72) have proposed methods of assessing clinical risk reclassification when the goal of analysis is risk prediction. They note that measures of risk reclassification are probably better than the c-statistic for assessing the value of adding a new marker to a prediction model.

Five studies (23, 33, 40, 43, 56) included an analysis that compared predictive models that used all Framingham risk factors, with and without CRP level, specifically among participants whose 10-year Framingham risk score categorized them as intermediate-risk. Three of the 5 (23, 33, 43) measured the c-statistic or the area under the receiver-operating characteristic curve. Only 1 study (23) used statistical analyses to compare the calibration of prediction models with and without CRP level. Using data from the Women's Health Study, Cook and colleagues (23) demonstrated that although measures of discrimination did not substantially differ between models with and without CRP level, a model that included CRP level had better fit, as measured by the Hosmer–Lemeshow calibration statistic. In that analysis, 14% of participants originally classified as intermediate-risk (10% to 20%) were reclassified as low-risk (<10%) and 5% were reclassified as high-risk (>20%). The actual 10-year risk was 19.9% for those reclassified as high-risk and 11.5% for those who remained intermediate-risk.

The other 4 studies used less rigorous analyses to assess the effect of CRP level on risk classification and did not measure calibration, with mixed results. Three studies (33, 40, 56) found that assessing CRP improved risk stratification specifically among intermediate-risk participants. In the Monitoring of Trends and Determinants in Cardiovascular Disease study (33), assessing CRP level in addition to the Framingham risk factors resulted in improved risk classification among participants with an initial 10-year risk of 11% to 19%. Among participants with a CRP level greater than 3.0 mg/L, some with an initial 10-year risk of 15% to 19% were reclassified as high-risk, whereas no participants with an initial 10-year risk of 11% to 14% were reclassified as high-risk. In an analysis of data from the Women's Health Study (40), CRP level was clearly predictive of incident cardiovascular disease among participants with 10-year Framingham risk scores between 10% and 20%. The risk for cardiovascular events was twice as high for those with CRP levels between 1.0 and 3.0 mg/L or between 3.0 and 10.0 mg/L than for those with levels less than 1.0 mg/L, although CIs were not reported. Similarly, in an analysis from the Cardiovascular Health Study, CRP level added to risk prediction among men at intermediate risk (56). Among men with a 10-year Framingham risk score between 10% and 20%, the observed 10-year incidence of CHD was 32% for those with CRP levels greater than 3.0 mg/L, compared with between 15% and 16% for those with CRP levels between 1.0 and 3.0 mg/L or less than 1.0 mg/L (56). In that cohort, however, CRP level did not add to risk prediction among intermediate-risk women. The negative study (43), an analysis from the Framingham cohort, estimated the 10-year risk for incident cardiovascular disease by tertile of CRP level among participants previously stratified as having a 10-year Framingham risk score between 10% and 20%. Tertile cut-points were 0.81 mg/L and 3.78 mg/L. The estimated 10-year risk did not significantly differ among the 3 CRP tertiles, and all 3 subgroups based on CRP level had an estimated 10-year risk in the intermediate range.

Previous Section Next Section

Discussion

The body of evidence that CRP level is independently associated with incident CHD is strong, with a risk ratio of 1.58 (CI, 1.37 to 1.83). Our search and systematic selection identified 23 studies of appropriate design from 24 cohorts. The aggregate quality of these studies is good to fair, and the body of evidence has no important inconsistency. We found no indication that the data from included studies were imprecise or sparse and no indication of high risk for reporting bias. We also noted some evidence of a dose–response gradient. These criteria support the conclusion of a strong body of evidence.

Previous meta-analyses (17–19) have found an association between CRP level and incident CHD. These meta-analyses were limited by their lack of a systematic basis for judging the validity of the evidence they used, and applicability to the target population and question of interest may be limited. Our systematic review and meta-analyses included more recent and updated studies, excluded studies of predominantly high-risk or low-risk populations, systematically rated the quality of all studies, and qualitatively appraised findings that are directly applicable to intermediate-risk patients.

The clinical implications of the association of CRP level with CHD events are less clear, because the pooled risk ratio does not necessarily measure the usefulness of CRP level in reclassifying intermediate-risk persons. The underlying studies did not directly assess whether the risk ratio for the overall sample applied to the intermediate-risk subgroup (for example, by looking for an interaction between the Framingham risk score and CRP levels). The strength of evidence from studies that attempted to measure the effect of using CRP level to improve risk classification among persons initially classified as intermediate-risk is moderate. Among intermediate-risk persons, subgroups with high CRP levels generally had a higher risk for coronary events than did those with average or low CRP levels.

In addition to multivariate regression analyses in prospective studies, many investigators (72–75) have advocated the use of other statistical methods to assess the incremental value of adding CRP level to global risk assessment. Several studies in our review (23, 33, 40, 42, 43, 50, 56, 58) compared predictive models that used all Framingham risk factors with and without a CRP level. Most of these used the change in the c-statistic or the area under the receiver-operating characteristic curve to compare the performance after adding CRP level. However, a marker can have a small effect on the c-statistic, a measure of discrimination, but be strongly related to risk as assessed in a multiple logistic or Cox regression model, or vice versa (76–78). Recent articles (24–26, 72) have discussed the limitations of the c-statistic and proposed methods of assessing clinical risk reclassification when risk prediction is the goal of analysis.

Relatively few studies have evaluated the effect of adding CRP level to reclassify initially intermediate-risk persons. Four studies in our review (33, 40, 43, 56) assessed differences in CHD risk among subgroups of intermediate-risk participants who were stratified by CRP level. Three of the 4 studies (33, 40, 56) found that those with higher CRP levels were at higher risk for CHD. However, their results are imprecise and their estimates are group averages, so they do not show how many persons would be reclassified as high-risk. A fifth study (23) calculated the risk reclassification when CRP level was added to a predictive model that included all Framingham risk score variables and found that the model with CRP level had better calibration to observed risk. In the negative study (43), researchers of the Framingham cohort concluded that CRP level does not seem to be beneficial for CHD risk assessment, particularly because adding CRP level to the risk model did not improve c-statistic results. Recently, these researchers reported a good-quality analysis of Framingham data (79) in which they calculated the risk reclassification of individual study participants when CRP level was added to traditional risk factors; including CRP level improved risk assessment by appropriately reclassifying a statistically significant percentage of incident CHD cases and noncases into higher or lower risk categories.

Although the types of analyses differed, 4 large, good-quality cohort studies are consistent in finding that assessing CRP level improves CHD risk stratification (23, 33, 40, 56, 79). These consistent findings provide moderately strong evidence that adding CRP level to risk models in intermediate-risk patients improves the identification of those at higher risk for incident CHD. However, additional research is needed to assess the effect of CRP level on risk reclassification of initially intermediate-risk persons and to statistically evaluate the calibration of prediction models to observed risk (26).

Establishing the independent predictive ability of a new risk factor is necessary but not sufficient for assessing its potential usefulness in screening for CHD risk. Other criteria must be considered, such as the prevalence of the factor in the target population, the reliability and cost of the test, potential harms of testing, and the effect that treatment for the risk factor has on modifying risk (80). C-reactive protein level favorably satisfies most of these criteria. National survey data suggest a prevalence of high CRP level of at least 20% to 25% among intermediate-risk persons (13, 81). Inexpensive, precise, high-sensitivity CRP serum assays are available (82, 83). Although considerable within-patient variation among CRP measurements has been reported (84), the reliability of 2 or 3 serial measurements is similar to that of a total cholesterol assay (84, 85). Weight loss, exercise, and smoking cessation can reduce serum CRP levels (86, 87), and lowering CRP levels with statin therapy in patients with acute coronary syndrome can lower their risk for recurrent myocardial infarction or coronary death (88). The viability of CRP as a new factor in global risk assessment for incident CHD is limited by sparse evidence that directly links therapeutic changes in CRP level to primary prevention of CHD events.

Results were recently published for JUPITER (Justification for the Use of Statins in Prevention: an Intervention Trial Evaluating Rosuvastatin), a good-quality randomized, controlled trial of rosuvastatin for primary prevention of cardiovascular events in 17 802 men and women with elevated (>2 mg/L) CRP levels, low-density lipoprotein cholesterol levels less than 3.4 mmol/L (<130 mg/dL) (median, 2.8 mmol/L [108 mg/dL]), and no other indication (such as diabetes) for statin therapy (89). Of 8901 participants who received 20 mg of rosuvastatin daily, 83 experienced first cardiovascular events (myocardial infarction, stroke, or death from cardiovascular causes) during the study period (median, 1.9 years), compared with 157 of 8901 participants in the placebo group, for a hazard ratio of 0.53 (CI, 0.40 to 0.69). By 1 year of follow-up, the median low-density lipoprotein cholesterol level was unchanged in participants receiving placebo and 1.4 mmol/L (55 mg/dL) in participants assigned to receive rosuvastatin. Rosuvastatin was also associated with an increased risk for physician-reported diabetes (3.0% vs. 2.4%).

Current guidelines recommend aggressive therapy only for high-risk patients, such as those with a Framingham risk score greater than 20%, diabetes, or known cardiovascular disease. Because approximately half of the patients in JUPITER had a Framingham risk score greater than 10%, these results provide evidence that 1 form of intensive risk reduction—aggressive lipid-lowering therapy—produces benefit for a population that includes intermediate-risk persons.

The implications of JUPITER for screening are less clear. JUPITER did not evaluate whether intermediate-risk patients who are reclassified as high-risk by using CRP level would benefit from treatment compared with intermediate-risk patients who are not reclassified. For example, the risk reduction from rosuvastatin therapy may have been as great in intermediate-risk participants who had CRP levels closer to the population average. The study also did not directly test whether lowering CRP levels reduced cardiac risk. Finally, JUPITER did not report rates of coronary events separately for low-risk and intermediate-risk persons. To fully understand the balance of benefits and harms associated with any particular form of intensive risk reduction intended for patients classified according to CRP levels, we also need to know the numbers needed to treat and the harms for different risk category subgroups. The length of follow-up was inadequate to fully evaluate the potential harms of aggressive statin therapy (90). When the trial was terminated, only 1076 (1 in 18) participants had 4 years of follow-up, and 2705 had 3 years of follow-up.

Other issues may influence guideline recommendations and merit discussion. Cross-sectional studies have found correlations between CRP level and traditional CHD risk factors (91), but the implications for the use of CRP in global risk assessment are not clear. The findings have been interpreted to mean that CRP level may represent a different aspect of risk, with complex interrelationships among CRP level, traditional risk factors, and CHD (91, 92). Others conclude that elevated CRP level is largely attributable to traditional risk factors, and CRP level “may have limited clinical utility as a screening tool” (13). In fact, the causal relationships between CRP level and traditional CHD risk factors are not clear (93). Correlation of CRP level with traditional risk factors does not preclude its potential association with CHD. The findings of many studies, including our meta-analyses, suggest that the degree of correlation between CRP level and traditional risk factors is not so great that CRP loses its independent effect. Although this statistical independence does not establish causality (94), it does support the potential use of CRP level as an adjunct in global risk assessment, particularly for targeted groups—such as intermediate-risk persons.

Our review has limitations. Studies used varying definitions, cutoffs, and methods of measurement for the Framingham risk factors and other cofactors. We accounted for these differences in our quality assessments and standardized our meta-analyses to recommended cut-off values. Because all studies were prospective, the likelihood of differential bias in measurement or reporting within studies is low. However, the net effect of the Framingham variables may vary from that of a calculated Framingham risk score for studies that did not measure each variable as defined for the Framingham risk score. In addition, although we distinguished those studies that completely adjusted for Framingham factors in our quality assessments and subgroup analyses, the inclusion of a nonuniform assortment of additional potential confounders might influence a study's relative risk estimate, with the net effect expected to be a reduction in the magnitude. Minority populations were poorly represented in most studies in our review. Ethnic and racial differences in biomarker levels (95, 96) and applicability of the Framingham risk score (97, 98) may limit the generalizability of our results.

In summary, our systematic review and meta-analyses indicate that CRP level is independently associated with incident CHD. The clinical implication of this finding is less clear, because the pooled risk ratio does not necessarily measure the usefulness of CRP level in reclassifying intermediate-risk persons. Although current evidence on the risk reclassification that would result from adding CRP level to a global risk score is promising, the strength of evidence from the 4 cohorts that attempted to measure the effect of using CRP among intermediate-risk persons is moderate. The viability of CRP as an adjunct to traditional factors is also uncertain because evidence linking changes in CRP level to primary prevention of CHD events is insufficient.

Previous Section Next Section

Article and Author Information

Acknowledgment: The authors thank Agency for Healthcare Research and Quality Medical Officer Janelle Guirguis-Blake, MD, for commenting on draft versions of the Systematic Evidence Synthesis (22) and the USPSTF members who served as leads for this project, including Kimberly D. Gregory, MD, MPH; Russell Harris, MD, MPH; George F. Sawaya, MD; and Barbara Yawn, MD, MSc. They also thank Andrew Hamilton, MLS, MS, for conducting the literature searches.
Grant Support: By the Agency for Healthcare Research and Quality (contract no. 290-02-0024, Task Order Number 2).
Potential Conflicts of Interest: None disclosed.
Requests for Single Reprints: David I. Buckley, MD, MPH, Oregon Health & Science University, Mailcode FM, 3181 Southwest Sam Jackson Park Road, Portland, OR 97239.
Current Author Addresses: Drs. Buckley, Fu, and Helfand: Oregon Health & Science University, Mailcode FM, 3181 Southwest Sam Jackson Park Road, Portland, OR 97239.
Ms. Freeman: Portland Veterans Affairs Medical Center, 3710 U.S. Veterans Hospital Road, Mailcode RD 71, Portland, OR 97239.
Dr. Rogers: 2150 South Main 511, Salt Lake City, UT 84115.
Author Contributions: Conception and design: D.I. Buckley, K. Rogers, M. Helfand.
Analysis and interpretation of the data: D.I. Buckley, R. Fu, M. Freeman, K. Rogers, M. Helfand.
Drafting of the article: D.I. Buckley, R. Fu, M. Helfand.
Critical revision of the article for important intellectual content: D.I. Buckley, R. Fu, M. Freeman, K. Rogers, M. Helfand.
Final approval of the article: D.I. Buckley, R. Fu, K. Rogers, M. Helfand.
Statistical expertise: R. Fu, M. Helfand.
Obtaining of funding: M. Helfand.
Administrative, technical, or logistic support: M. Freeman, M. Helfand.
Collection and assembly of data: D.I. Buckley, R. Fu, K. Rogers, M. Helfand.

Previous Section

References

1.↵
1. FerdinandKC
Coronary artery disease in minority racial and ethnic groups in the United States.Am J Cardiol20069712A-19Apmid:16442932
Ferdinand KC. Coronary artery disease in minority racial and ethnic groups in the United States. Am J Cardiol. 2006;97:12A-19A. [PMID: 16442932]
Medline Web of Science
2.↵
1. WilsonPW,
2. D'AgostinoRB,
3. LevyD,
4. BelangerAM,
5. SilbershatzH,
6. KannelWB
Prediction of coronary heart disease using risk factor categories.Circulation1998971837-47pmid:9603539
Wilson PW, D'Agostino RB, Levy D, Belanger AM, Silbershatz H, Kannel WB. Prediction of coronary heart disease using risk factor categories. Circulation. 1998;97:1837-47. [PMID: 9603539]
Abstract/FREE Full Text
3.↵
1. McGillHC, Jr,
2. McMahanCA,
3. MalcomGT,
4. OalmannMC,
5. StrongJP
Effects of serum lipoproteins and smoking on atherosclerosis in young men and women. The PDAY Research Group. Pathobiological Determinants of Atherosclerosis in Youth.Arterioscler Thromb Vasc Biol19971795-106pmid:9012643
McGill HC Jr, McMahan CA, Malcom GT, Oalmann MC, Strong JP. Effects of serum lipoproteins and smoking on atherosclerosis in young men and women. The PDAY Research Group. Pathobiological Determinants of Atherosclerosis in Youth. Arterioscler Thromb Vasc Biol. 1997;17:95-106. [PMID: 9012643]
Abstract/FREE Full Text
4.↵
1. GreenlandP,
2. KnollMD,
3. StamlerJ,
4. NeatonJD,
5. DyerAR,
6. GarsideDB
et al.Major risk factors as antecedents of fatal and nonfatal coronary heart disease events.JAMA2003290891-7pmid:12928465
Greenland P, Knoll MD, Stamler J, Neaton JD, Dyer AR, Garside DB, et al. Major risk factors as antecedents of fatal and nonfatal coronary heart disease events. JAMA. 2003;290:891-7. [PMID: 12928465]
Abstract/FREE Full Text
5.↵
1. KhotUN,
2. KhotMB,
3. BajzerCT,
4. SappSK,
5. OhmanEM,
6. BrenerSJ
et al.Prevalence of conventional risk factors in patients with coronary heart disease.JAMA2003290898-904pmid:12928466
Khot UN, Khot MB, Bajzer CT, Sapp SK, Ohman EM, Brener SJ, et al. Prevalence of conventional risk factors in patients with coronary heart disease. JAMA. 2003;290:898-904. [PMID: 12928466]
Abstract/FREE Full Text
6.↵
1. SmithSC, Jr
Current and future directions of cardiovascular risk prediction.Am J Cardiol20069728A-32Apmid:16442934
Smith SC Jr. Current and future directions of cardiovascular risk prediction. Am J Cardiol. 2006;97:28A-32A. [PMID: 16442934]
CrossRef Medline
7.↵
1. RossR
Atherosclerosis—an inflammatory disease.N Engl J Med1999340115-26pmid:9887164
Ross R. Atherosclerosis—an inflammatory disease. N Engl J Med. 1999;340:115-26. [PMID: 9887164]
FREE Full Text
8.↵
1. RidkerPM,
2. HennekensCH,
3. BuringJE,
4. RifaiN
C-reactive protein and other markers of inflammation in the prediction of cardiovascular disease in women.N Engl J Med2000342836-43pmid:10733371
Ridker PM, Hennekens CH, Buring JE, Rifai N. C-reactive protein and other markers of inflammation in the prediction of cardiovascular disease in women. N Engl J Med. 2000;342:836-43. [PMID: 10733371]
Abstract/FREE Full Text
9.↵
1. PepysMB,
2. HirschfieldGM
C-reactive protein: a critical update.J Clin Invest20031111805-12pmid:12813013
Pepys MB, Hirschfield GM. C-reactive protein: a critical update. J Clin Invest. 2003;111:1805-12. [PMID: 12813013]
CrossRef Medline Web of Science
10.↵

Scirica BM, Morrow DA. Is C-reactive protein an innocent bystander or proatherogenic culprit? The verdict is still out. Circulation. 2006;113:2128-34; discussion 2151. [PMID: 16651484]
11.↵
1. HingoraniAD,
2. ShahT,
3. CasasJP
Linking observational and genetic approaches to determine the role of C-reactive protein in heart disease risk [Editorial].Eur Heart J2006271261-3pmid:16684780
Hingorani AD, Shah T, Casas JP. Linking observational and genetic approaches to determine the role of C-reactive protein in heart disease risk [Editorial]. Eur Heart J. 2006;27:1261-3. [PMID: 16684780]
FREE Full Text
12.↵
1. LemieuxI,
2. PascotA,
3. Prud'hommeD,
4. AlmérasN,
5. BogatyP,
6. NadeauA
et al.Elevated C-reactive protein: another component of the atherothrombotic profile of abdominal obesity.Arterioscler Thromb Vasc Biol200121961-7pmid:11397704
Lemieux I, Pascot A, Prud'homme D, Alméras N, Bogaty P, Nadeau A, et al. Elevated C-reactive protein: another component of the atherothrombotic profile of abdominal obesity. Arterioscler Thromb Vasc Biol. 2001;21:961-7. [PMID: 11397704]
Abstract/FREE Full Text
13.↵
1. MillerM,
2. ZhanM,
3. HavasS
High attributable risk of elevated C-reactive protein level to conventional coronary heart disease risk factors: the Third National Health and Nutrition Examination Survey.Arch Intern Med20051652063-8pmid:16216995
Miller M, Zhan M, Havas S. High attributable risk of elevated C-reactive protein level to conventional coronary heart disease risk factors: the Third National Health and Nutrition Examination Survey. Arch Intern Med. 2005;165:2063-8. [PMID: 16216995]
Abstract/FREE Full Text
14.↵
1. PearsonTA,
2. MensahGA,
3. AlexanderRW,
4. AndersonJL,
5. CannonRO, 3rd,
6. CriquiM
et al.Centers for Disease Control and PreventionMarkers of inflammation and cardiovascular disease: application to clinical and public health practice: A statement for healthcare professionals from the Centers for Disease Control and Prevention and the American Heart Association.Circulation2003107499-511pmid:12551878
Pearson TA, Mensah GA, Alexander RW, Anderson JL, Cannon RO 3rd, Criqui M, et al; Centers for Disease Control and Prevention. Markers of inflammation and cardiovascular disease: application to clinical and public health practice: A statement for healthcare professionals from the Centers for Disease Control and Prevention and the American Heart Association. Circulation. 2003;107:499-511. [PMID: 12551878]
FREE Full Text
15.↵
1. PasternakRC,
2. AbramsJ,
3. GreenlandP,
4. SmahaLA,
5. WilsonPW,
6. Houston-MillerN
34th Bethesda Conference: Task force 1—Identification of coronary heart disease risk: is there a detection gap?J Am Coll Cardiol2003411863-74pmid:12798553
Pasternak RC, Abrams J, Greenland P, Smaha LA, Wilson PW, Houston-Miller N. 34th Bethesda Conference: Task force 1—Identification of coronary heart disease risk: is there a detection gap? J Am Coll Cardiol. 2003;41:1863-74. [PMID: 12798553]
FREE Full Text
16.↵
1. GrundySM,
2. BazzarreT,
3. CleemanJ,
4. D'AgostinoRB, Sr,
5. HillM,
6. Houston-MillerN
et al.Prevention Conference V: Beyond secondary prevention: identifying the high-risk patient for primary prevention: medical office assessment: Writing Group I.Circulation20001013-E11pmid:10618316
Grundy SM, Bazzarre T, Cleeman J, D'Agostino RB Sr, Hill M, Houston-Miller N, et al. Prevention Conference V: Beyond secondary prevention: identifying the high-risk patient for primary prevention: medical office assessment: Writing Group I. Circulation. 2000;101:E3-E11. [PMID: 10618316]
FREE Full Text
17.↵
1. DaneshJ,
2. CollinsR,
3. ApplebyP,
4. PetoR
Association of fibrinogen, C-reactive protein, albumin, or leukocyte count with coronary heart disease: meta-analyses of prospective studies.JAMA19982791477-82pmid:9600484
Danesh J, Collins R, Appleby P, Peto R. Association of fibrinogen, C-reactive protein, albumin, or leukocyte count with coronary heart disease: meta-analyses of prospective studies. JAMA. 1998;279:1477-82. [PMID: 9600484]
Abstract/FREE Full Text
18.↵
1. DaneshJ,
2. WhincupP,
3. WalkerM,
4. LennonL,
5. ThomsonA,
6. ApplebyP
et al.Low grade inflammation and coronary heart disease: prospective study and updated meta-analyses.BMJ2000321199-204pmid:10903648
Danesh J, Whincup P, Walker M, Lennon L, Thomson A, Appleby P, et al. Low grade inflammation and coronary heart disease: prospective study and updated meta-analyses. BMJ. 2000;321:199-204. [PMID: 10903648]
Abstract/FREE Full Text
19.↵
1. DaneshJ,
2. WheelerJG,
3. HirschfieldGM,
4. EdaS,
5. EiriksdottirG,
6. RumleyA
et al.C-reactive protein and other circulating markers of inflammation in the prediction of coronary heart disease.N Engl J Med20043501387-97pmid:15070788
Danesh J, Wheeler JG, Hirschfield GM, Eda S, Eiriksdottir G, Rumley A, et al. C-reactive protein and other circulating markers of inflammation in the prediction of coronary heart disease. N Engl J Med. 2004;350:1387-97. [PMID: 15070788]
Abstract/FREE Full Text
20.↵
1. HarrisRP,
2. HelfandM,
3. WoolfSH,
4. LohrKN,
5. MulrowCD,
6. TeutschSM
et al.Methods Work GroupThird US Preventive Services Task ForceCurrent methods of the US Preventive Services Task Force: a review of the process.Am J Prev Med20012021-35pmid:11306229
Harris RP, Helfand M, Woolf SH, Lohr KN, Mulrow CD, Teutsch SM, et al; Methods Work Group, Third US Preventive Services Task Force. Current methods of the US Preventive Services Task Force: a review of the process. Am J Prev Med. 2001;20:21-35. [PMID: 11306229]
Medline
21.↵
1. GuyattGH,
2. OxmanAD,
3. VistGE,
4. KunzR,
5. Falck-YtterY,
6. Alonso-CoelloP
et al.GRADE Working GroupGRADE: an emerging consensus on rating quality of evidence and strength of recommendations.BMJ2008336924-6pmid:18436948
Guyatt GH, Oxman AD, Vist GE, Kunz R, Falck-Ytter Y, Alonso-Coello P, et al; GRADE Working Group. GRADE: an emerging consensus on rating quality of evidence and strength of recommendations. BMJ. 2008;336:924-6. [PMID: 18436948]
FREE Full Text
22.↵
1. HelfandM,
2. BuckleyD,
3. FlemingC,
4. FuR,
5. FreemanM,
6. HumphreyL
et al.Screening for Intermediate Risk Factors for Coronary Heart Disease: Systematic Evidence Synthesis. Evidence Synthesis No. 73. AHRQ Publication No. 09-05137-EF-1.Rockville, MDAgency for Healthcare Research and Quality2009
Helfand M, Buckley D, Fleming C, Fu R, Freeman M, Humphrey L, et al. Screening for Intermediate Risk Factors for Coronary Heart Disease: Systematic Evidence Synthesis. Evidence Synthesis No. 73. AHRQ Publication No. 09-05137-EF-1. Rockville, MD: Agency for Healthcare Research and Quality; 2009.
23.↵
1. CookNR,
2. BuringJE,
3. RidkerPM
The effect of including C-reactive protein in cardiovascular risk prediction models for women.Ann Intern Med200614521-9pmid:16818925
Cook NR, Buring JE, Ridker PM. The effect of including C-reactive protein in cardiovascular risk prediction models for women. Ann Intern Med. 2006;145:21-9. [PMID: 16818925]
Abstract/FREE Full Text
24.↵
1. JanesH,
2. PepeMS,
3. GuW
Assessing the value of risk predictions by using risk stratification tables.Ann Intern Med2008149751-60pmid:19017593
Janes H, Pepe MS, Gu W. Assessing the value of risk predictions by using risk stratification tables. Ann Intern Med. 2008;149:751-60. [PMID: 19017593]
Abstract/FREE Full Text
25.↵

Pencina MJ, D'Agostino RB Sr, D'Agostino RB Jr, Vasan RS. Evaluating the added predictive ability of a new marker: from area under the ROC curve to reclassification and beyond. Stat Med. 2008;27:157-72; discussion 207-12. [PMID: 17569110]
26.↵
1. CookNR
Statistical evaluation of prognostic versus diagnostic models: beyond the ROC curve.Clin Chem20085417-23pmid:18024533
Cook NR. Statistical evaluation of prognostic versus diagnostic models: beyond the ROC curve. Clin Chem. 2008;54:17-23. [PMID: 18024533]
Abstract/FREE Full Text
27.↵
1. KoenigW,
2. SundM,
3. FröhlichM,
4. FischerHG,
5. LöwelH,
6. DöringA
et al.C-Reactive protein, a sensitive marker of inflammation, predicts future risk of coronary heart disease in initially healthy middle-aged men: results from the MONICA (Monitoring Trends and Determinants in Cardiovascular Disease) Augsburg Cohort Study, 1984 to 1992.Circulation199999237-42pmid:9892589
Koenig W, Sund M, Fröhlich M, Fischer HG, Löwel H, Döring A, et al. C-Reactive protein, a sensitive marker of inflammation, predicts future risk of coronary heart disease in initially healthy middle-aged men: results from the MONICA (Monitoring Trends and Determinants in Cardiovascular Disease) Augsburg Cohort Study, 1984 to 1992. Circulation. 1999;99:237-42. [PMID: 9892589]
Abstract/FREE Full Text
28.↵
1. ParkR,
2. DetranoR,
3. XiangM,
4. FuP,
5. IbrahimY,
6. LaBreeL
et al.Combined use of computed tomography coronary calcium scores and C-reactive protein levels in predicting cardiovascular events in nondiabetic individuals.Circulation20021062073-7pmid:12379576
Park R, Detrano R, Xiang M, Fu P, Ibrahim Y, LaBree L, et al. Combined use of computed tomography coronary calcium scores and C-reactive protein levels in predicting cardiovascular events in nondiabetic individuals. Circulation. 2002;106:2073-7. [PMID: 12379576]
Abstract/FREE Full Text
29.↵
1. DerSimonianR,
2. LairdN
Meta-analysis in clinical trials.Control Clin Trials19867177-88pmid:3802833
DerSimonian R, Laird N. Meta-analysis in clinical trials. Control Clin Trials. 1986;7:177-88. [PMID: 3802833]
CrossRef Medline Web of Science
30.↵
1. HigginsJP,
2. ThompsonSG
Quantifying heterogeneity in a meta-analysis.Stat Med2002211539-58pmid:12111919
Higgins JP, Thompson SG. Quantifying heterogeneity in a meta-analysis. Stat Med. 2002;21:1539-58. [PMID: 12111919]
CrossRef Medline Web of Science
31.↵
1. EggerM,
2. Davey SmithG,
3. SchneiderM,
4. MinderC
Bias in meta-analysis detected by a simple, graphical test.BMJ1997315629-34pmid:9310563
Egger M, Davey Smith G, Schneider M, Minder C. Bias in meta-analysis detected by a simple, graphical test. BMJ. 1997;315:629-34. [PMID: 9310563]
Abstract/FREE Full Text
32.↵
1. BlakeGJ,
2. RifaiN,
3. BuringJE,
4. RidkerPM
Blood pressure, C-reactive protein, and risk of future cardiovascular events.Circulation20031082993-9pmid:14638538
Blake GJ, Rifai N, Buring JE, Ridker PM. Blood pressure, C-reactive protein, and risk of future cardiovascular events. Circulation. 2003;108:2993-9. [PMID: 14638538]
Abstract/FREE Full Text
33.↵
1. KoenigW,
2. LöwelH,
3. BaumertJ,
4. MeisingerC
C-reactive protein modulates risk prediction based on the Framingham Score: implications for future risk assessment: results from a large cohort study in southern Germany.Circulation20041091349-53pmid:15023871
Koenig W, Löwel H, Baumert J, Meisinger C. C-reactive protein modulates risk prediction based on the Framingham Score: implications for future risk assessment: results from a large cohort study in southern Germany. Circulation. 2004;109:1349-53. [PMID: 15023871]
Abstract/FREE Full Text
34.↵
1. KoenigW,
2. KhuseyinovaN,
3. LöwelH,
4. TrischlerG,
5. MeisingerC
Lipoprotein-associated phospholipase A2 adds to risk prediction of incident coronary events by C-reactive protein in apparently healthy middle-aged men from the general population: results from the 14-year follow-up of a large cohort from southern Germany.Circulation20041101903-8pmid:15451783
Koenig W, Khuseyinova N, Löwel H, Trischler G, Meisinger C. Lipoprotein-associated phospholipase A2 adds to risk prediction of incident coronary events by C-reactive protein in apparently healthy middle-aged men from the general population: results from the 14-year follow-up of a large cohort from southern Germany. Circulation. 2004;110:1903-8. [PMID: 15451783]
Abstract/FREE Full Text
35.↵
1. LawlorDA,
2. SmithGD,
3. RumleyA,
4. LoweGD,
5. EbrahimS
Associations of fibrinogen and C-reactive protein with prevalent and incident coronary heart disease are attenuated by adjustment for confounding factors. British Women's Heart and Health Study.Thromb Haemost200593955-63pmid:15886815
Lawlor DA, Smith GD, Rumley A, Lowe GD, Ebrahim S. Associations of fibrinogen and C-reactive protein with prevalent and incident coronary heart disease are attenuated by adjustment for confounding factors. British Women's Heart and Health Study. Thromb Haemost. 2005;93:955-63. [PMID: 15886815]
Medline Web of Science
36.↵
1. LoweGD,
2. YarnellJW,
3. RumleyA,
4. BaintonD,
5. SweetnamPM
C-reactive protein, fibrin D-dimer, and incident ischemic heart disease in the Speedwell study: are inflammation and fibrin turnover linked in pathogenesis?Arterioscler Thromb Vasc Biol200121603-10pmid:11304479
Lowe GD, Yarnell JW, Rumley A, Bainton D, Sweetnam PM. C-reactive protein, fibrin D-dimer, and incident ischemic heart disease in the Speedwell study: are inflammation and fibrin turnover linked in pathogenesis? Arterioscler Thromb Vasc Biol. 2001;21:603-10. [PMID: 11304479]
Abstract/FREE Full Text
37.↵
1. LoweGD,
2. SweetnamPM,
3. YarnellJW,
4. RumleyA,
5. RumleyC,
6. BaintonD
et al.C-reactive protein, fibrin d-dimer, and risk of ischemic heart disease: the Caerphilly and Speedwell studies.Arterioscler Thromb Vasc Biol2004241957-62pmid:15308549
Lowe GD, Sweetnam PM, Yarnell JW, Rumley A, Rumley C, Bainton D, et al. C-reactive protein, fibrin d-dimer, and risk of ischemic heart disease: the Caerphilly and Speedwell studies. Arterioscler Thromb Vasc Biol. 2004;24:1957-62. [PMID: 15308549]
Abstract/FREE Full Text
38.↵
1. PirroM,
2. BergeronJ,
3. DagenaisGR,
4. BernardPM,
5. CantinB,
6. DesprésJP
et al.Age and duration of follow-up as modulators of the risk for ischemic heart disease associated with high plasma C-reactive protein levels in men.Arch Intern Med20011612474-80pmid:11700160
Pirro M, Bergeron J, Dagenais GR, Bernard PM, Cantin B, Després JP, et al. Age and duration of follow-up as modulators of the risk for ischemic heart disease associated with high plasma C-reactive protein levels in men. Arch Intern Med. 2001;161:2474-80. [PMID: 11700160]
Abstract/FREE Full Text
39.↵
1. RidkerPM,
2. RifaiN,
3. CookNR,
4. BradwinG,
5. BuringJE
Non-HDL cholesterol, apolipoproteins A-I and B100, standard lipid measures, lipid ratios, and CRP as risk factors for cardiovascular disease in women.JAMA2005294326-33pmid:16030277
Ridker PM, Rifai N, Cook NR, Bradwin G, Buring JE. Non-HDL cholesterol, apolipoproteins A-I and B100, standard lipid measures, lipid ratios, and CRP as risk factors for cardiovascular disease in women. JAMA. 2005;294:326-33. [PMID: 16030277]
Abstract/FREE Full Text
40.↵
1. RidkerPM,
2. CookN
Clinical usefulness of very high and very low levels of C-reactive protein across the full range of Framingham Risk Scores.Circulation20041091955-9pmid:15051634
Ridker PM, Cook N. Clinical usefulness of very high and very low levels of C-reactive protein across the full range of Framingham Risk Scores. Circulation. 2004;109:1955-9. [PMID: 15051634]
Abstract/FREE Full Text
41.↵
1. RidkerPM,
2. RifaiN,
3. RoseL,
4. BuringJE,
5. CookNR
Comparison of C-reactive protein and low-density lipoprotein cholesterol levels in the prediction of first cardiovascular events.N Engl J Med20023471557-65pmid:12432042
Ridker PM, Rifai N, Rose L, Buring JE, Cook NR. Comparison of C-reactive protein and low-density lipoprotein cholesterol levels in the prediction of first cardiovascular events. N Engl J Med. 2002;347:1557-65. [PMID: 12432042]
Abstract/FREE Full Text
42.↵
1. St-PierreAC,
2. CantinB,
3. BergeronJ,
4. PirroM,
5. DagenaisGR,
6. DesprésJP
et al.Inflammatory markers and long-term risk of ischemic heart disease in men A 13-year follow-up of the Quebec Cardiovascular Study.Atherosclerosis2005182315-21pmid:16159604
St-Pierre AC, Cantin B, Bergeron J, Pirro M, Dagenais GR, Després JP, et al. Inflammatory markers and long-term risk of ischemic heart disease in men A 13-year follow-up of the Quebec Cardiovascular Study. Atherosclerosis. 2005;182:315-21. [PMID: 16159604]
CrossRef Medline Web of Science
43.↵
1. WilsonPW,
2. NamBH,
3. PencinaM,
4. D'AgostinoRB, Sr,
5. BenjaminEJ,
6. O'DonnellCJ
C-reactive protein and risk of cardiovascular disease in men and women from the Framingham Heart Study.Arch Intern Med20051652473-8pmid:16314543
Wilson PW, Nam BH, Pencina M, D'Agostino RB Sr, Benjamin EJ, O'Donnell CJ. C-reactive protein and risk of cardiovascular disease in men and women from the Framingham Heart Study. Arch Intern Med. 2005;165:2473-8. [PMID: 16314543]
Abstract/FREE Full Text
44.↵
1. LucG,
2. BardJM,
3. Juhan-VagueI,
4. FerrieresJ,
5. EvansA,
6. AmouyelP
et al.PRIME Study GroupC-reactive protein, interleukin-6, and fibrinogen as predictors of coronary heart disease: the PRIME Study.Arterioscler Thromb Vasc Biol2003231255-61pmid:12775578
Luc G, Bard JM, Juhan-Vague I, Ferrieres J, Evans A, Amouyel P, et al; PRIME Study Group. C-reactive protein, interleukin-6, and fibrinogen as predictors of coronary heart disease: the PRIME Study. Arterioscler Thromb Vasc Biol. 2003;23:1255-61. [PMID: 12775578]
Abstract/FREE Full Text
45.↵
1. PaiJK,
2. PischonT,
3. MaJ,
4. MansonJE,
5. HankinsonSE,
6. JoshipuraK
et al.Inflammatory markers and the risk of coronary heart disease in men and women.N Engl J Med20043512599-610pmid:15602020
Pai JK, Pischon T, Ma J, Manson JE, Hankinson SE, Joshipura K, et al. Inflammatory markers and the risk of coronary heart disease in men and women. N Engl J Med. 2004;351:2599-610. [PMID: 15602020]
Abstract/FREE Full Text
46.↵
1. PradhanAD,
2. MansonJE,
3. RossouwJE,
4. SiscovickDS,
5. MoutonCP,
6. RifaiN
et al.Inflammatory biomarkers, hormone replacement therapy, and incident coronary heart disease: prospective analysis from the Women's Health Initiative observational study.JAMA2002288980-7pmid:12190368
Pradhan AD, Manson JE, Rossouw JE, Siscovick DS, Mouton CP, Rifai N, et al. Inflammatory biomarkers, hormone replacement therapy, and incident coronary heart disease: prospective analysis from the Women's Health Initiative observational study. JAMA. 2002;288:980-7. [PMID: 12190368]
Abstract/FREE Full Text
47.↵
1. RidkerPM,
2. BuringJE,
3. ShihJ,
4. MatiasM,
5. HennekensCH
Prospective study of C-reactive protein and the risk of future cardiovascular events among apparently healthy women.Circulation199898731-3pmid:9727541
Ridker PM, Buring JE, Shih J, Matias M, Hennekens CH. Prospective study of C-reactive protein and the risk of future cardiovascular events among apparently healthy women. Circulation. 1998;98:731-3. [PMID: 9727541]
Abstract/FREE Full Text
48.↵
1. RidkerPM,
2. CushmanM,
3. StampferMJ,
4. TracyRP,
5. HennekensCH
Inflammation, aspirin, and the risk of cardiovascular disease in apparently healthy men.N Engl J Med1997336973-9pmid:9077376
Ridker PM, Cushman M, Stampfer MJ, Tracy RP, Hennekens CH. Inflammation, aspirin, and the risk of cardiovascular disease in apparently healthy men. N Engl J Med. 1997;336:973-9. [PMID: 9077376]
Abstract/FREE Full Text
49.↵
1. RifaiN,
2. BuringJE,
3. LeeIM,
4. MansonJE,
5. RidkerPM
Is C-reactive protein specific for vascular disease in women?Ann Intern Med2002136529-33pmid:11926788
Rifai N, Buring JE, Lee IM, Manson JE, Ridker PM. Is C-reactive protein specific for vascular disease in women? Ann Intern Med. 2002;136:529-33. [PMID: 11926788]
Abstract/FREE Full Text
50.↵
1. van der MeerIM,
2. de MaatMP,
3. KiliaanAJ,
4. van der KuipDA,
5. HofmanA,
6. WittemanJC
The value of C-reactive protein in cardiovascular risk prediction: the Rotterdam Study.Arch Intern Med20031631323-8pmid:12796068
van der Meer IM, de Maat MP, Kiliaan AJ, van der Kuip DA, Hofman A, Witteman JC. The value of C-reactive protein in cardiovascular risk prediction: the Rotterdam Study. Arch Intern Med. 2003;163:1323-8. [PMID: 12796068]
Abstract/FREE Full Text
51.↵
1. WitherellHL,
2. SmithKL,
3. FriedmanGD,
4. LeyC,
5. ThomDH,
6. OrentreichN
et al.C-reactive protein, Helicobacter pylori, Chlamydia pneumoniae, cytomegalovirus and risk for myocardial infarction.Ann Epidemiol200313170-7pmid:12604160
Witherell HL, Smith KL, Friedman GD, Ley C, Thom DH, Orentreich N, et al. C-reactive protein, Helicobacter pylori, Chlamydia pneumoniae, cytomegalovirus and risk for myocardial infarction. Ann Epidemiol. 2003;13:170-7. [PMID: 12604160]
CrossRef Medline Web of Science
52.↵
1. BallantyneCM,
2. HoogeveenRC,
3. BangH,
4. CoreshJ,
5. FolsomAR,
6. HeissG
et al.Lipoprotein-associated phospholipase A2, high-sensitivity C-reactive protein, and risk for incident coronary heart disease in middle-aged men and women in the Atherosclerosis Risk in Communities (ARIC) study.Circulation2004109837-42pmid:14757686
Ballantyne CM, Hoogeveen RC, Bang H, Coresh J, Folsom AR, Heiss G, et al. Lipoprotein-associated phospholipase A2, high-sensitivity C-reactive protein, and risk for incident coronary heart disease in middle-aged men and women in the Atherosclerosis Risk in Communities (ARIC) study. Circulation. 2004;109:837-42. [PMID: 14757686]
Abstract/FREE Full Text
53.↵
1. FolsomAR,
2. AleksicN,
3. CatellierD,
4. JunejaHS,
5. WuKK
C-reactive protein and incident coronary heart disease in the Atherosclerosis Risk In Communities (ARIC) study.Am Heart J2002144233-8pmid:12177639
Folsom AR, Aleksic N, Catellier D, Juneja HS, Wu KK. C-reactive protein and incident coronary heart disease in the Atherosclerosis Risk In Communities (ARIC) study. Am Heart J. 2002;144:233-8. [PMID: 12177639]
CrossRef Medline Web of Science
54.↵
1. GramJ,
2. BladbjergEM,
3. MøllerL,
4. SjølA,
5. JespersenJ
Tissue-type plasminogen activator and C-reactive protein in acute coronary heart disease. A nested case-control study.J Intern Med2000247205-12pmid:10692083
Gram J, Bladbjerg EM, Møller L, Sjøl A, Jespersen J. Tissue-type plasminogen activator and C-reactive protein in acute coronary heart disease. A nested case-control study. J Intern Med. 2000;247:205-12. [PMID: 10692083]
CrossRef Medline Web of Science
55.↵
1. BoekholdtSM,
2. HackCE,
3. SandhuMS,
4. LubenR,
5. BinghamSA,
6. WarehamNJ
et al.C-reactive protein levels and coronary artery disease incidence and mortality in apparently healthy men and women: the EPIC-Norfolk prospective population study 1993-2003.Atherosclerosis2006187415-22pmid:16257408
Boekholdt SM, Hack CE, Sandhu MS, Luben R, Bingham SA, Wareham NJ, et al. C-reactive protein levels and coronary artery disease incidence and mortality in apparently healthy men and women: the EPIC-Norfolk prospective population study 1993-2003. Atherosclerosis. 2006;187:415-22. [PMID: 16257408]
CrossRef Medline Web of Science
56.↵
1. CushmanM,
2. ArnoldAM,
3. PsatyBM,
4. ManolioTA,
5. KullerLH,
6. BurkeGL
et al.C-reactive protein and the 10-year incidence of coronary heart disease in older men and women: the cardiovascular health study.Circulation200511225-31pmid:15983251
Cushman M, Arnold AM, Psaty BM, Manolio TA, Kuller LH, Burke GL, et al. C-reactive protein and the 10-year incidence of coronary heart disease in older men and women: the cardiovascular health study. Circulation. 2005;112:25-31. [PMID: 15983251]
Abstract/FREE Full Text
57.↵
1. EverettBM,
2. KurthT,
3. BuringJE,
4. RidkerPM
The relative strength of C-reactive protein and lipid levels as determinants of ischemic stroke compared with coronary heart disease in women.J Am Coll Cardiol2006482235-42pmid:17161253
Everett BM, Kurth T, Buring JE, Ridker PM. The relative strength of C-reactive protein and lipid levels as determinants of ischemic stroke compared with coronary heart disease in women. J Am Coll Cardiol. 2006;48:2235-42. [PMID: 17161253]
Abstract/FREE Full Text
58.↵
1. FolsomAR,
2. ChamblessLE,
3. BallantyneCM,
4. CoreshJ,
5. HeissG,
6. WuKK
et al.An assessment of incremental coronary risk prediction using C-reactive protein and other novel risk markers: the atherosclerosis risk in communities study.Arch Intern Med20061661368-73pmid:16832001
Folsom AR, Chambless LE, Ballantyne CM, Coresh J, Heiss G, Wu KK, et al. An assessment of incremental coronary risk prediction using C-reactive protein and other novel risk markers: the atherosclerosis risk in communities study. Arch Intern Med. 2006;166:1368-73. [PMID: 16832001]
Abstract/FREE Full Text
59.↵
1. KoenigW,
2. KhuseyinovaN,
3. BaumertJ,
4. ThorandB,
5. LoewelH,
6. ChamblessL
et al.Increased concentrations of C-reactive protein and IL-6 but not IL-18 are independently associated with incident coronary events in middle-aged men and women: results from the MONICA/KORA Augsburg case-cohort study, 1984-2002.Arterioscler Thromb Vasc Biol2006262745-51pmid:17008587
Koenig W, Khuseyinova N, Baumert J, Thorand B, Loewel H, Chambless L, et al. Increased concentrations of C-reactive protein and IL-6 but not IL-18 are independently associated with incident coronary events in middle-aged men and women: results from the MONICA/KORA Augsburg case-cohort study, 1984-2002. Arterioscler Thromb Vasc Biol. 2006;26:2745-51. [PMID: 17008587]
Abstract/FREE Full Text
60.↵
1. MoraS,
2. RifaiN,
3. BuringJE,
4. RidkerPM
Additive value of immunoassay-measured fibrinogen and high-sensitivity C-reactive protein levels for predicting incident cardiovascular events.Circulation2006114381-7pmid:16864722
Mora S, Rifai N, Buring JE, Ridker PM. Additive value of immunoassay-measured fibrinogen and high-sensitivity C-reactive protein levels for predicting incident cardiovascular events. Circulation. 2006;114:381-7. [PMID: 16864722]
Abstract/FREE Full Text
61.↵
1. PischonT,
2. MöhligM,
3. HoffmannK,
4. SprangerJ,
5. WeikertC,
6. WillichSN
et al.Comparison of relative and attributable risk of myocardial infarction and stroke according to C-reactive protein and low-density lipoprotein cholesterol levels.Eur J Epidemiol200722429-38pmid:17557140
Pischon T, Möhlig M, Hoffmann K, Spranger J, Weikert C, Willich SN, et al. Comparison of relative and attributable risk of myocardial infarction and stroke according to C-reactive protein and low-density lipoprotein cholesterol levels. Eur J Epidemiol. 2007;22:429-38. [PMID: 17557140]
CrossRef Medline
62.↵
1. TuomistoK,
2. JousilahtiP,
3. SundvallJ,
4. PajunenP,
5. SalomaaV
C-reactive protein, interleukin-6 and tumor necrosis factor alpha as predictors of incident coronary and cardiovascular events and total mortality. A population-based, prospective study.Thromb Haemost200695511-8pmid:16525580
Tuomisto K, Jousilahti P, Sundvall J, Pajunen P, Salomaa V. C-reactive protein, interleukin-6 and tumor necrosis factor alpha as predictors of incident coronary and cardiovascular events and total mortality. A population-based, prospective study. Thromb Haemost. 2006;95:511-8. [PMID: 16525580]
Medline Web of Science
63.↵
1. TzoulakiI,
2. MurrayGD,
3. LeeAJ,
4. RumleyA,
5. LoweGD,
6. FowkesFG
Relative value of inflammatory, hemostatic, and rheological factors for incident myocardial infarction and stroke: the Edinburgh Artery Study.Circulation20071152119-27pmid:17404162
Tzoulaki I, Murray GD, Lee AJ, Rumley A, Lowe GD, Fowkes FG. Relative value of inflammatory, hemostatic, and rheological factors for incident myocardial infarction and stroke: the Edinburgh Artery Study. Circulation. 2007;115:2119-27. [PMID: 17404162]
Abstract/FREE Full Text
64.↵
1. KullerLH,
2. TracyRP,
3. ShatenJ,
4. MeilahnEN
Relation of C-reactive protein and coronary heart disease in the MRFIT nested case-control study. Multiple Risk Factor Intervention Trial.Am J Epidemiol1996144537-47pmid:8797513
Kuller LH, Tracy RP, Shaten J, Meilahn EN. Relation of C-reactive protein and coronary heart disease in the MRFIT nested case-control study. Multiple Risk Factor Intervention Trial. Am J Epidemiol. 1996;144:537-47. [PMID: 8797513]
Abstract/FREE Full Text
65.↵
1. AgewallS,
2. WikstrandJ,
3. FagerbergB
Prothrombin fragment 1 + 2 is a risk factor for myocardial infarction in treated hypertensive men.J Hypertens199816537-41pmid:9797200
Agewall S, Wikstrand J, Fagerberg B. Prothrombin fragment 1 + 2 is a risk factor for myocardial infarction in treated hypertensive men. J Hypertens. 1998;16:537-41. [PMID: 9797200]
CrossRef Medline Web of Science
66.↵
1. RoivainenM,
2. Viik-KajanderM,
3. PalosuoT,
4. ToivanenP,
5. LeinonenM,
6. SaikkuP
et al.Infections, inflammation, and the risk of coronary heart disease.Circulation2000101252-7pmid:10645920
Roivainen M, Viik-Kajander M, Palosuo T, Toivanen P, Leinonen M, Saikku P, et al. Infections, inflammation, and the risk of coronary heart disease. Circulation. 2000;101:252-7. [PMID: 10645920]
Abstract/FREE Full Text
67.↵
1. StrandbergTE,
2. TilvisRS
C-reactive protein, cardiovascular risk factors, and mortality in a prospective study in the elderly.Arterioscler Thromb Vasc Biol2000201057-60pmid:10764673
Strandberg TE, Tilvis RS. C-reactive protein, cardiovascular risk factors, and mortality in a prospective study in the elderly. Arterioscler Thromb Vasc Biol. 2000;20:1057-60. [PMID: 10764673]
Abstract/FREE Full Text
68.↵
1. PackardCJ,
2. O'ReillyDS,
3. CaslakeMJ,
4. McMahonAD,
5. FordI,
6. CooneyJ
et al.Lipoprotein-associated phospholipase A2 as an independent predictor of coronary heart disease. West of Scotland Coronary Prevention Study Group.N Engl J Med20003431148-55pmid:11036120
Packard CJ, O'Reilly DS, Caslake MJ, McMahon AD, Ford I, Cooney J, et al. Lipoprotein-associated phospholipase A2 as an independent predictor of coronary heart disease. West of Scotland Coronary Prevention Study Group. N Engl J Med. 2000;343:1148-55. [PMID: 11036120]
Abstract/FREE Full Text
69.↵
1. RidkerPM
High-sensitivity C-reactive protein: potential adjunct for global risk assessment in the primary prevention of cardiovascular disease.Circulation20011031813-8pmid:11282915
Ridker PM. High-sensitivity C-reactive protein: potential adjunct for global risk assessment in the primary prevention of cardiovascular disease. Circulation. 2001;103:1813-8. [PMID: 11282915]
Abstract/FREE Full Text
70.↵
1. HarrisTB,
2. FerrucciL,
3. TracyRP,
4. CortiMC,
5. WacholderS,
6. EttingerWH, Jr
et al.Associations of elevated interleukin-6 and C-reactive protein levels with mortality in the elderly.Am J Med1999106506-12pmid:10335721
Harris TB, Ferrucci L, Tracy RP, Corti MC, Wacholder S, Ettinger WH Jr, et al. Associations of elevated interleukin-6 and C-reactive protein levels with mortality in the elderly. Am J Med. 1999;106:506-12. [PMID: 10335721]
CrossRef Medline Web of Science
71.↵
1. JagerA,
2. van HinsberghVW,
3. KostensePJ,
4. EmeisJJ,
5. YudkinJS,
6. NijpelsG
et al.von Willebrand factor, C-reactive protein, and 5-year mortality in diabetic and nondiabetic subjects: the Hoorn Study.Arterioscler Thromb Vasc Biol1999193071-8pmid:10591689
Jager A, van Hinsbergh VW, Kostense PJ, Emeis JJ, Yudkin JS, Nijpels G, et al. von Willebrand factor, C-reactive protein, and 5-year mortality in diabetic and nondiabetic subjects: the Hoorn Study. Arterioscler Thromb Vasc Biol. 1999;19:3071-8. [PMID: 10591689]
Abstract/FREE Full Text
72.↵
1. CookNR
Use and misuse of the receiver operating characteristic curve in risk prediction.Circulation2007115928-35pmid:17309939
Cook NR. Use and misuse of the receiver operating characteristic curve in risk prediction. Circulation. 2007;115:928-35. [PMID: 17309939]
Abstract/FREE Full Text
73.↵
1. GreenlandP,
2. O'MalleyPG
When is a new prediction marker useful? A consideration of lipoprotein-associated phospholipase A2 and C-reactive protein for stroke risk [Editorial].Arch Intern Med20051652454-6pmid:16314539
Greenland P, O'Malley PG. When is a new prediction marker useful? A consideration of lipoprotein-associated phospholipase A2 and C-reactive protein for stroke risk [Editorial]. Arch Intern Med. 2005;165:2454-6. [PMID: 16314539]
FREE Full Text
74.↵
1. Lloyd-JonesDM,
2. LiuK,
3. TianL,
4. GreenlandP
Narrative review: Assessment of C-reactive protein in risk prediction for cardiovascular disease.Ann Intern Med200614535-42pmid:16818927
Lloyd-Jones DM, Liu K, Tian L, Greenland P. Narrative review: Assessment of C-reactive protein in risk prediction for cardiovascular disease. Ann Intern Med. 2006;145:35-42. [PMID: 16818927]
Abstract/FREE Full Text
75.↵
1. KoenigW
Cardiovascular biomarkers: added value with an integrated approach? [Editorial].Circulation20071163-5pmid:17606853
Koenig W. Cardiovascular biomarkers: added value with an integrated approach? [Editorial]. Circulation. 2007;116:3-5. [PMID: 17606853]
FREE Full Text
76.↵
1. PepeMS,
2. JanesH,
3. LongtonG,
4. LeisenringW,
5. NewcombP
Limitations of the odds ratio in gauging the performance of a diagnostic, prognostic, or screening marker.Am J Epidemiol2004159882-90pmid:15105181
Pepe MS, Janes H, Longton G, Leisenring W, Newcomb P. Limitations of the odds ratio in gauging the performance of a diagnostic, prognostic, or screening marker. Am J Epidemiol. 2004;159:882-90. [PMID: 15105181]
Abstract/FREE Full Text
77.↵
1. MoonsKG,
2. HarrellFE
Sensitivity and specificity should be de-emphasized in diagnostic accuracy studies.Acad Radiol200310670-2pmid:12809422
Moons KG, Harrell FE. Sensitivity and specificity should be de-emphasized in diagnostic accuracy studies. Acad Radiol. 2003;10:670-2. [PMID: 12809422]
CrossRef Medline Web of Science
78.↵
1. PepeMS,
2. FengZ,
3. HuangY,
4. LongtonG,
5. PrenticeR,
6. ThompsonIM
et al.Integrating the predictiveness of a marker with its performance as a classifier.Am J Epidemiol2008167362-8pmid:17982157
Pepe MS, Feng Z, Huang Y, Longton G, Prentice R, Thompson IM, et al. Integrating the predictiveness of a marker with its performance as a classifier. Am J Epidemiol. 2008;167:362-8. [PMID: 17982157]
Abstract/FREE Full Text
79.↵
1. WilsonPWF,
2. PencinaMJ,
3. JacquesP,
4. SelhubJ,
5. D'AgostinoRB,
6. O'DonnellCJ
C-reactive protein and reclassification of cardiovascular risk in the Framingham Heart Study.Circ Cardiovasc Qual Outcomes2008192-97
Wilson PWF, Pencina MJ, Jacques P, Selhub J, D'Agostino RB, O'Donnell CJ. C-reactive protein and reclassification of cardiovascular risk in the Framingham Heart Study. Circ Cardiovasc Qual Outcomes. 2008;1:92-97.
80.↵

National Cholesterol Education Program (NCEP) Expert Panel on Detection, Evaluation, and Treatment of High Blood Cholesterol in Adults (Adult Treatment Panel III)Third Report of the National Cholesterol Education Program (NCEP) Expert Panel on Detection, Evaluation, and Treatment of High Blood Cholesterol in Adults (Adult Treatment Panel III) final report.Circulation20021063143-421pmid:12485966
National Cholesterol Education Program (NCEP) Expert Panel on Detection, Evaluation, and Treatment of High Blood Cholesterol in Adults (Adult Treatment Panel III). Third Report of the National Cholesterol Education Program (NCEP) Expert Panel on Detection, Evaluation, and Treatment of High Blood Cholesterol in Adults (Adult Treatment Panel III) final report. Circulation. 2002;106:3143-421. [PMID: 12485966]

FREE Full Text
81.↵
1. AjaniUA,
2. FordES,
3. MokdadAH
Prevalence of high C-reactive protein in persons with serum lipid concentrations within recommended values.Clin Chem2004501618-22pmid:15205370
Ajani UA, Ford ES, Mokdad AH. Prevalence of high C-reactive protein in persons with serum lipid concentrations within recommended values. Clin Chem. 2004;50:1618-22. [PMID: 15205370]
Abstract/FREE Full Text
82.↵
1. HutchinsonWL,
2. KoenigW,
3. FröhlichM,
4. SundM,
5. LoweGD,
6. PepysMB
Immunoradiometric assay of circulating C-reactive protein: age-related values in the adult general population.Clin Chem200046934-8pmid:10894836
Hutchinson WL, Koenig W, Fröhlich M, Sund M, Lowe GD, Pepys MB. Immunoradiometric assay of circulating C-reactive protein: age-related values in the adult general population. Clin Chem. 2000;46:934-8. [PMID: 10894836]
Abstract/FREE Full Text
83.↵
1. WilkinsJ,
2. GallimoreJR,
3. MooreEG,
4. PepysMB
Rapid automated high sensitivity enzyme immunoassay of C-reactive protein.Clin Chem1998441358-61pmid:9625071
Wilkins J, Gallimore JR, Moore EG, Pepys MB. Rapid automated high sensitivity enzyme immunoassay of C-reactive protein. Clin Chem. 1998;44:1358-61. [PMID: 9625071]
FREE Full Text
84.↵
1. KoenigW,
2. SundM,
3. FröhlichM,
4. LöwelH,
5. HutchinsonWL,
6. PepysMB
Refinement of the association of serum C-reactive protein concentration and coronary heart disease risk by correction for within-subject variation over time: the MONICA Augsburg studies, 1984 and 1987.Am J Epidemiol2003158357-64pmid:12915501
Koenig W, Sund M, Fröhlich M, Löwel H, Hutchinson WL, Pepys MB. Refinement of the association of serum C-reactive protein concentration and coronary heart disease risk by correction for within-subject variation over time: the MONICA Augsburg studies, 1984 and 1987. Am J Epidemiol. 2003;158:357-64. [PMID: 12915501]
Abstract/FREE Full Text
85.↵
1. OckeneIS,
2. MatthewsCE,
3. RifaiN,
4. RidkerPM,
5. ReedG,
6. StanekE
Variability and classification accuracy of serial high-sensitivity C-reactive protein measurements in healthy adults.Clin Chem200147444-50pmid:11238295
Ockene IS, Matthews CE, Rifai N, Ridker PM, Reed G, Stanek E. Variability and classification accuracy of serial high-sensitivity C-reactive protein measurements in healthy adults. Clin Chem. 2001;47:444-50. [PMID: 11238295]
Abstract/FREE Full Text
86.↵
1. NicklasBJ,
2. YouT,
3. PahorM
Behavioural treatments for chronic systemic inflammation: effects of dietary weight loss and exercise training.CMAJ20051721199-209pmid:15851714
Nicklas BJ, You T, Pahor M. Behavioural treatments for chronic systemic inflammation: effects of dietary weight loss and exercise training. CMAJ. 2005;172:1199-209. [PMID: 15851714]
Abstract/FREE Full Text
87.↵
1. NissenSE,
2. TuzcuEM,
3. SchoenhagenP,
4. CroweT,
5. SasielaWJ,
6. TsaiJ
et al.Reversal of Atherosclerosis with Aggressive Lipid Lowering (REVERSAL) InvestigatorsStatin therapy, LDL cholesterol, C-reactive protein, and coronary artery disease.N Engl J Med200535229-38pmid:15635110
Nissen SE, Tuzcu EM, Schoenhagen P, Crowe T, Sasiela WJ, Tsai J, et al; Reversal of Atherosclerosis with Aggressive Lipid Lowering (REVERSAL) Investigators. Statin therapy, LDL cholesterol, C-reactive protein, and coronary artery disease. N Engl J Med. 2005;352:29-38. [PMID: 15635110]
Abstract/FREE Full Text
88.↵
1. RidkerPM,
2. CannonCP,
3. MorrowD,
4. RifaiN,
5. RoseLM,
6. McCabeCH
et al.Pravastatin or Atorvastatin Evaluation and Infection Therapy-Thrombolysis in Myocardial Infarction 22 (PROVE IT-TIMI 22) InvestigatorsC-reactive protein levels and outcomes after statin therapy.N Engl J Med200535220-8pmid:15635109
Ridker PM, Cannon CP, Morrow D, Rifai N, Rose LM, McCabe CH, et al; Pravastatin or Atorvastatin Evaluation and Infection Therapy-Thrombolysis in Myocardial Infarction 22 (PROVE IT-TIMI 22) Investigators. C-reactive protein levels and outcomes after statin therapy. N Engl J Med. 2005;352:20-8. [PMID: 15635109]
Abstract/FREE Full Text
89.↵
1. RidkerPM,
2. DanielsonE,
3. FonsecaFA,
4. GenestJ,
5. GottoAM, Jr,
6. KasteleinJJ
et al.JUPITER Study GroupRosuvastatin to prevent vascular events in men and women with elevated C-reactive protein.N Engl J Med20083592195-207pmid:18997196
Ridker PM, Danielson E, Fonseca FA, Genest J, Gotto AM Jr, Kastelein JJ, et al; JUPITER Study Group. Rosuvastatin to prevent vascular events in men and women with elevated C-reactive protein. N Engl J Med. 2008;359:2195-207. [PMID: 18997196]
Abstract/FREE Full Text
90.↵
1. HlatkyMA
Expanding the orbit of primary prevention—moving beyond JUPITER [Editorial].N Engl J Med20083592280-2pmid:18997195
Hlatky MA. Expanding the orbit of primary prevention—moving beyond JUPITER [Editorial]. N Engl J Med. 2008;359:2280-2. [PMID: 18997195]
FREE Full Text
91.↵
1. AlbertMA,
2. GlynnRJ,
3. RidkerPM
Plasma concentration of C-reactive protein and the calculated Framingham Coronary Heart Disease Risk Score.Circulation2003108161-5pmid:12835213
Albert MA, Glynn RJ, Ridker PM. Plasma concentration of C-reactive protein and the calculated Framingham Coronary Heart Disease Risk Score. Circulation. 2003;108:161-5. [PMID: 12835213]
Abstract/FREE Full Text
92.↵
1. BermudezEA,
2. RifaiN,
3. BuringJ,
4. MansonJE,
5. RidkerPM
Interrelationships among circulating interleukin-6, C-reactive protein, and traditional cardiovascular risk factors in women.Arterioscler Thromb Vasc Biol2002221668-73pmid:12377747
Bermudez EA, Rifai N, Buring J, Manson JE, Ridker PM. Interrelationships among circulating interleukin-6, C-reactive protein, and traditional cardiovascular risk factors in women. Arterioscler Thromb Vasc Biol. 2002;22:1668-73. [PMID: 12377747]
Abstract/FREE Full Text
93.↵

Engström G. The role of inflammation for heart disease risk cannot be determined by correlations between C-reactive protein and risk factors [Letter]. Arch Intern Med. 2006;166:1040; author reply 1040-1. [PMID: 16682580]
94.↵
1. BrotmanDJ,
2. WalkerE,
3. LauerMS,
4. O'BrienRG
In search of fewer independent risk factors.Arch Intern Med2005165138-45pmid:15668358
Brotman DJ, Walker E, Lauer MS, O'Brien RG. In search of fewer independent risk factors. Arch Intern Med. 2005;165:138-45. [PMID: 15668358]
Abstract/FREE Full Text
95.↵
1. HowardBV,
2. Le,
3. BelcherJD,
4. FlackJM,
5. JacobsDR, Jr,
6. LewisCE
et al.Concentrations of Lp(a) in black and white young adults: relations to risk factors for cardiovascular disease.Ann Epidemiol19944341-50pmid:7981840
Howard BV, Le NA, Belcher JD, Flack JM, Jacobs DR Jr, Lewis CE, et al. Concentrations of Lp(a) in black and white young adults: relations to risk factors for cardiovascular disease. Ann Epidemiol. 1994;4:341-50. [PMID: 7981840]
Medline
96.↵
1. WangW,
2. HuD,
3. LeeET,
4. FabsitzRR,
5. WeltyTK,
6. RobbinsDC
et al.Lipoprotein(a) in American Indians is low and not independently associated with cardiovascular disease. The Strong Heart Study.Ann Epidemiol200212107-14pmid:11880218
Wang W, Hu D, Lee ET, Fabsitz RR, Welty TK, Robbins DC, et al. Lipoprotein(a) in American Indians is low and not independently associated with cardiovascular disease. The Strong Heart Study. Ann Epidemiol. 2002;12:107-14. [PMID: 11880218]
CrossRef Medline Web of Science
97.↵
1. D'AgostinoRB, Sr,
2. GrundyS,
3. SullivanLM,
4. WilsonP
CHD Risk Prediction GroupValidation of the Framingham coronary heart disease prediction scores: results of a multiple ethnic groups investigation.JAMA2001286180-7pmid:11448281
D'Agostino RB Sr, Grundy S, Sullivan LM, Wilson P; CHD Risk Prediction Group. Validation of the Framingham coronary heart disease prediction scores: results of a multiple ethnic groups investigation. JAMA. 2001;286:180-7. [PMID: 11448281]
Abstract/FREE Full Text
98.↵
1. LiuJ,
2. HongY,
3. D'AgostinoRB, Sr,
4. WuZ,
5. WangW,
6. SunJ
et al.Predictive value for the Chinese population of the Framingham CHD risk assessment tool compared with the Chinese Multi-Provincial Cohort Study.JAMA20042912591-9pmid:15173150
Liu J, Hong Y, D'Agostino RB Sr, Wu Z, Wang W, Sun J, et al. Predictive value for the Chinese population of the Framingham CHD risk assessment tool compared with the Chinese Multi-Provincial Cohort Study. JAMA. 2004;291:2591-9. [PMID: 15173150]
Abstract/FREE Full Text

[1] 1.↵

FerdinandKC

Coronary artery disease in minority racial and ethnic groups in the United States.Am J Cardiol20069712A-19Apmid:16442932
Ferdinand KC. Coronary artery disease in minority racial and ethnic groups in the United States. Am J Cardiol. 2006;97:12A-19A. [PMID: 16442932]

Medline Web of Science

[2] FerdinandKC

[3] 2.↵

WilsonPW,

D'AgostinoRB,

LevyD,

BelangerAM,

SilbershatzH,

KannelWB

Prediction of coronary heart disease using risk factor categories.Circulation1998971837-47pmid:9603539
Wilson PW, D'Agostino RB, Levy D, Belanger AM, Silbershatz H, Kannel WB. Prediction of coronary heart disease using risk factor categories. Circulation. 1998;97:1837-47. [PMID: 9603539]

Abstract/FREE Full Text

[4] WilsonPW,

[5] D'AgostinoRB,

[6] LevyD,

[7] BelangerAM,

[8] SilbershatzH,

[9] KannelWB

[10] 3.↵

McGillHC, Jr,

McMahanCA,

MalcomGT,

OalmannMC,

StrongJP

Effects of serum lipoproteins and smoking on atherosclerosis in young men and women. The PDAY Research Group. Pathobiological Determinants of Atherosclerosis in Youth.Arterioscler Thromb Vasc Biol19971795-106pmid:9012643
McGill HC Jr, McMahan CA, Malcom GT, Oalmann MC, Strong JP. Effects of serum lipoproteins and smoking on atherosclerosis in young men and women. The PDAY Research Group. Pathobiological Determinants of Atherosclerosis in Youth. Arterioscler Thromb Vasc Biol. 1997;17:95-106. [PMID: 9012643]

Abstract/FREE Full Text

[11] McGillHC, Jr,

[12] McMahanCA,

[13] MalcomGT,

[14] OalmannMC,

[15] StrongJP

[16] 4.↵

GreenlandP,

KnollMD,

StamlerJ,

NeatonJD,

DyerAR,

GarsideDB

et al.Major risk factors as antecedents of fatal and nonfatal coronary heart disease events.JAMA2003290891-7pmid:12928465
Greenland P, Knoll MD, Stamler J, Neaton JD, Dyer AR, Garside DB, et al. Major risk factors as antecedents of fatal and nonfatal coronary heart disease events. JAMA. 2003;290:891-7. [PMID: 12928465]

Abstract/FREE Full Text

[17] GreenlandP,

[18] KnollMD,

[19] StamlerJ,

[20] NeatonJD,

[21] DyerAR,

[22] GarsideDB

[23] 5.↵

KhotUN,

KhotMB,

BajzerCT,

SappSK,

OhmanEM,

BrenerSJ

et al.Prevalence of conventional risk factors in patients with coronary heart disease.JAMA2003290898-904pmid:12928466
Khot UN, Khot MB, Bajzer CT, Sapp SK, Ohman EM, Brener SJ, et al. Prevalence of conventional risk factors in patients with coronary heart disease. JAMA. 2003;290:898-904. [PMID: 12928466]

Abstract/FREE Full Text

[24] KhotUN,

[25] KhotMB,

[26] BajzerCT,

[27] SappSK,

[28] OhmanEM,

[29] BrenerSJ

[30] 6.↵

SmithSC, Jr

Current and future directions of cardiovascular risk prediction.Am J Cardiol20069728A-32Apmid:16442934
Smith SC Jr. Current and future directions of cardiovascular risk prediction. Am J Cardiol. 2006;97:28A-32A. [PMID: 16442934]

CrossRef Medline

[31] SmithSC, Jr

[32] 7.↵

RossR

Atherosclerosis—an inflammatory disease.N Engl J Med1999340115-26pmid:9887164
Ross R. Atherosclerosis—an inflammatory disease. N Engl J Med. 1999;340:115-26. [PMID: 9887164]

FREE Full Text

[33] RossR

[34] 8.↵

RidkerPM,

HennekensCH,

BuringJE,

RifaiN

C-reactive protein and other markers of inflammation in the prediction of cardiovascular disease in women.N Engl J Med2000342836-43pmid:10733371
Ridker PM, Hennekens CH, Buring JE, Rifai N. C-reactive protein and other markers of inflammation in the prediction of cardiovascular disease in women. N Engl J Med. 2000;342:836-43. [PMID: 10733371]

Abstract/FREE Full Text

[35] RidkerPM,

[36] HennekensCH,

[37] BuringJE,

[38] RifaiN

[39] 9.↵

PepysMB,

HirschfieldGM

C-reactive protein: a critical update.J Clin Invest20031111805-12pmid:12813013
Pepys MB, Hirschfield GM. C-reactive protein: a critical update. J Clin Invest. 2003;111:1805-12. [PMID: 12813013]

CrossRef Medline Web of Science

[40] PepysMB,

[41] HirschfieldGM

[42] 10.↵

Scirica BM, Morrow DA. Is C-reactive protein an innocent bystander or proatherogenic culprit? The verdict is still out. Circulation. 2006;113:2128-34; discussion 2151. [PMID: 16651484]

[43] 11.↵

HingoraniAD,

ShahT,

CasasJP

Linking observational and genetic approaches to determine the role of C-reactive protein in heart disease risk [Editorial].Eur Heart J2006271261-3pmid:16684780
Hingorani AD, Shah T, Casas JP. Linking observational and genetic approaches to determine the role of C-reactive protein in heart disease risk [Editorial]. Eur Heart J. 2006;27:1261-3. [PMID: 16684780]

FREE Full Text

[44] HingoraniAD,

[45] ShahT,

[46] CasasJP

[47] 12.↵

LemieuxI,

PascotA,

Prud'hommeD,

AlmérasN,

BogatyP,

NadeauA

et al.Elevated C-reactive protein: another component of the atherothrombotic profile of abdominal obesity.Arterioscler Thromb Vasc Biol200121961-7pmid:11397704
Lemieux I, Pascot A, Prud'homme D, Alméras N, Bogaty P, Nadeau A, et al. Elevated C-reactive protein: another component of the atherothrombotic profile of abdominal obesity. Arterioscler Thromb Vasc Biol. 2001;21:961-7. [PMID: 11397704]

Abstract/FREE Full Text

[48] LemieuxI,

[49] PascotA,

[50] Prud'hommeD,

[51] AlmérasN,

[52] BogatyP,

[53] NadeauA

[54] 13.↵

MillerM,

ZhanM,

HavasS

High attributable risk of elevated C-reactive protein level to conventional coronary heart disease risk factors: the Third National Health and Nutrition Examination Survey.Arch Intern Med20051652063-8pmid:16216995
Miller M, Zhan M, Havas S. High attributable risk of elevated C-reactive protein level to conventional coronary heart disease risk factors: the Third National Health and Nutrition Examination Survey. Arch Intern Med. 2005;165:2063-8. [PMID: 16216995]

Abstract/FREE Full Text

[55] MillerM,

[56] ZhanM,

[57] HavasS

[58] 14.↵

PearsonTA,

MensahGA,

AlexanderRW,

AndersonJL,

CannonRO, 3rd,

CriquiM

et al.Centers for Disease Control and PreventionMarkers of inflammation and cardiovascular disease: application to clinical and public health practice: A statement for healthcare professionals from the Centers for Disease Control and Prevention and the American Heart Association.Circulation2003107499-511pmid:12551878
Pearson TA, Mensah GA, Alexander RW, Anderson JL, Cannon RO 3rd, Criqui M, et al; Centers for Disease Control and Prevention. Markers of inflammation and cardiovascular disease: application to clinical and public health practice: A statement for healthcare professionals from the Centers for Disease Control and Prevention and the American Heart Association. Circulation. 2003;107:499-511. [PMID: 12551878]

FREE Full Text

[59] PearsonTA,

[60] MensahGA,

[61] AlexanderRW,

[62] AndersonJL,

[63] CannonRO, 3rd,

[64] CriquiM

[65] 15.↵

PasternakRC,

AbramsJ,

GreenlandP,

SmahaLA,

WilsonPW,

Houston-MillerN

34th Bethesda Conference: Task force 1—Identification of coronary heart disease risk: is there a detection gap?J Am Coll Cardiol2003411863-74pmid:12798553
Pasternak RC, Abrams J, Greenland P, Smaha LA, Wilson PW, Houston-Miller N. 34th Bethesda Conference: Task force 1—Identification of coronary heart disease risk: is there a detection gap? J Am Coll Cardiol. 2003;41:1863-74. [PMID: 12798553]

FREE Full Text

[66] PasternakRC,

[67] AbramsJ,

[68] GreenlandP,

[69] SmahaLA,

[70] WilsonPW,

[71] Houston-MillerN

[72] 16.↵

GrundySM,

BazzarreT,

CleemanJ,

D'AgostinoRB, Sr,

HillM,

Houston-MillerN

et al.Prevention Conference V: Beyond secondary prevention: identifying the high-risk patient for primary prevention: medical office assessment: Writing Group I.Circulation20001013-E11pmid:10618316
Grundy SM, Bazzarre T, Cleeman J, D'Agostino RB Sr, Hill M, Houston-Miller N, et al. Prevention Conference V: Beyond secondary prevention: identifying the high-risk patient for primary prevention: medical office assessment: Writing Group I. Circulation. 2000;101:E3-E11. [PMID: 10618316]

FREE Full Text

[73] GrundySM,

[74] BazzarreT,

[75] CleemanJ,

[76] D'AgostinoRB, Sr,

[77] HillM,

[78] Houston-MillerN

[79] 17.↵

DaneshJ,

CollinsR,

ApplebyP,

PetoR

Association of fibrinogen, C-reactive protein, albumin, or leukocyte count with coronary heart disease: meta-analyses of prospective studies.JAMA19982791477-82pmid:9600484
Danesh J, Collins R, Appleby P, Peto R. Association of fibrinogen, C-reactive protein, albumin, or leukocyte count with coronary heart disease: meta-analyses of prospective studies. JAMA. 1998;279:1477-82. [PMID: 9600484]

Abstract/FREE Full Text

[80] DaneshJ,

[81] CollinsR,

[82] ApplebyP,

[83] PetoR

[84] 18.↵

DaneshJ,

WhincupP,

WalkerM,

LennonL,

ThomsonA,

ApplebyP

et al.Low grade inflammation and coronary heart disease: prospective study and updated meta-analyses.BMJ2000321199-204pmid:10903648
Danesh J, Whincup P, Walker M, Lennon L, Thomson A, Appleby P, et al. Low grade inflammation and coronary heart disease: prospective study and updated meta-analyses. BMJ. 2000;321:199-204. [PMID: 10903648]

Abstract/FREE Full Text

[85] DaneshJ,

[86] WhincupP,

[87] WalkerM,

[88] LennonL,

[89] ThomsonA,

[90] ApplebyP

[91] 19.↵

DaneshJ,

WheelerJG,

HirschfieldGM,

EdaS,

EiriksdottirG,

RumleyA

et al.C-reactive protein and other circulating markers of inflammation in the prediction of coronary heart disease.N Engl J Med20043501387-97pmid:15070788
Danesh J, Wheeler JG, Hirschfield GM, Eda S, Eiriksdottir G, Rumley A, et al. C-reactive protein and other circulating markers of inflammation in the prediction of coronary heart disease. N Engl J Med. 2004;350:1387-97. [PMID: 15070788]

Abstract/FREE Full Text

[92] DaneshJ,

[93] WheelerJG,

[94] HirschfieldGM,

[95] EdaS,

[96] EiriksdottirG,

[97] RumleyA

[98] 20.↵

HarrisRP,

HelfandM,

WoolfSH,

LohrKN,

MulrowCD,

TeutschSM

et al.Methods Work GroupThird US Preventive Services Task ForceCurrent methods of the US Preventive Services Task Force: a review of the process.Am J Prev Med20012021-35pmid:11306229
Harris RP, Helfand M, Woolf SH, Lohr KN, Mulrow CD, Teutsch SM, et al; Methods Work Group, Third US Preventive Services Task Force. Current methods of the US Preventive Services Task Force: a review of the process. Am J Prev Med. 2001;20:21-35. [PMID: 11306229]

Medline

[99] HarrisRP,

[100] HelfandM,

[101] WoolfSH,

[102] LohrKN,

[103] MulrowCD,

[104] TeutschSM

[105] 21.↵

GuyattGH,

OxmanAD,

VistGE,

KunzR,

Falck-YtterY,

Alonso-CoelloP

et al.GRADE Working GroupGRADE: an emerging consensus on rating quality of evidence and strength of recommendations.BMJ2008336924-6pmid:18436948
Guyatt GH, Oxman AD, Vist GE, Kunz R, Falck-Ytter Y, Alonso-Coello P, et al; GRADE Working Group. GRADE: an emerging consensus on rating quality of evidence and strength of recommendations. BMJ. 2008;336:924-6. [PMID: 18436948]

FREE Full Text

[106] GuyattGH,

[107] OxmanAD,

[108] VistGE,

[109] KunzR,

[110] Falck-YtterY,

[111] Alonso-CoelloP

[112] 22.↵

HelfandM,

BuckleyD,

FlemingC,

FuR,

FreemanM,

HumphreyL

et al.Screening for Intermediate Risk Factors for Coronary Heart Disease: Systematic Evidence Synthesis. Evidence Synthesis No. 73. AHRQ Publication No. 09-05137-EF-1.Rockville, MDAgency for Healthcare Research and Quality2009
Helfand M, Buckley D, Fleming C, Fu R, Freeman M, Humphrey L, et al. Screening for Intermediate Risk Factors for Coronary Heart Disease: Systematic Evidence Synthesis. Evidence Synthesis No. 73. AHRQ Publication No. 09-05137-EF-1. Rockville, MD: Agency for Healthcare Research and Quality; 2009.

[113] HelfandM,

[114] BuckleyD,

[115] FlemingC,

[116] FuR,

[117] FreemanM,

[118] HumphreyL

[119] 23.↵

CookNR,

BuringJE,

RidkerPM

The effect of including C-reactive protein in cardiovascular risk prediction models for women.Ann Intern Med200614521-9pmid:16818925
Cook NR, Buring JE, Ridker PM. The effect of including C-reactive protein in cardiovascular risk prediction models for women. Ann Intern Med. 2006;145:21-9. [PMID: 16818925]

Abstract/FREE Full Text

[120] CookNR,

[121] BuringJE,

[122] RidkerPM

[123] 24.↵

JanesH,

PepeMS,

GuW

Assessing the value of risk predictions by using risk stratification tables.Ann Intern Med2008149751-60pmid:19017593
Janes H, Pepe MS, Gu W. Assessing the value of risk predictions by using risk stratification tables. Ann Intern Med. 2008;149:751-60. [PMID: 19017593]

Abstract/FREE Full Text

[124] JanesH,

[125] PepeMS,

[126] GuW

[127] 25.↵

Pencina MJ, D'Agostino RB Sr, D'Agostino RB Jr, Vasan RS. Evaluating the added predictive ability of a new marker: from area under the ROC curve to reclassification and beyond. Stat Med. 2008;27:157-72; discussion 207-12. [PMID: 17569110]

[128] 26.↵

CookNR

Statistical evaluation of prognostic versus diagnostic models: beyond the ROC curve.Clin Chem20085417-23pmid:18024533
Cook NR. Statistical evaluation of prognostic versus diagnostic models: beyond the ROC curve. Clin Chem. 2008;54:17-23. [PMID: 18024533]

Abstract/FREE Full Text

[129] CookNR

[130] 27.↵

KoenigW,

SundM,

FröhlichM,

FischerHG,

LöwelH,

DöringA

et al.C-Reactive protein, a sensitive marker of inflammation, predicts future risk of coronary heart disease in initially healthy middle-aged men: results from the MONICA (Monitoring Trends and Determinants in Cardiovascular Disease) Augsburg Cohort Study, 1984 to 1992.Circulation199999237-42pmid:9892589
Koenig W, Sund M, Fröhlich M, Fischer HG, Löwel H, Döring A, et al. C-Reactive protein, a sensitive marker of inflammation, predicts future risk of coronary heart disease in initially healthy middle-aged men: results from the MONICA (Monitoring Trends and Determinants in Cardiovascular Disease) Augsburg Cohort Study, 1984 to 1992. Circulation. 1999;99:237-42. [PMID: 9892589]

Abstract/FREE Full Text

[131] KoenigW,

[132] SundM,

[133] FröhlichM,

[134] FischerHG,

[135] LöwelH,

[136] DöringA

[137] 28.↵

ParkR,

DetranoR,

XiangM,

FuP,

IbrahimY,

LaBreeL

et al.Combined use of computed tomography coronary calcium scores and C-reactive protein levels in predicting cardiovascular events in nondiabetic individuals.Circulation20021062073-7pmid:12379576
Park R, Detrano R, Xiang M, Fu P, Ibrahim Y, LaBree L, et al. Combined use of computed tomography coronary calcium scores and C-reactive protein levels in predicting cardiovascular events in nondiabetic individuals. Circulation. 2002;106:2073-7. [PMID: 12379576]

Abstract/FREE Full Text

[138] ParkR,

[139] DetranoR,

[140] XiangM,

[141] FuP,

[142] IbrahimY,

[143] LaBreeL

[144] 29.↵

DerSimonianR,

LairdN

Meta-analysis in clinical trials.Control Clin Trials19867177-88pmid:3802833
DerSimonian R, Laird N. Meta-analysis in clinical trials. Control Clin Trials. 1986;7:177-88. [PMID: 3802833]

CrossRef Medline Web of Science

[145] DerSimonianR,

[146] LairdN

[147] 30.↵

HigginsJP,

ThompsonSG

Quantifying heterogeneity in a meta-analysis.Stat Med2002211539-58pmid:12111919
Higgins JP, Thompson SG. Quantifying heterogeneity in a meta-analysis. Stat Med. 2002;21:1539-58. [PMID: 12111919]

CrossRef Medline Web of Science

[148] HigginsJP,

[149] ThompsonSG

[150] 31.↵

EggerM,

Davey SmithG,

SchneiderM,

MinderC

Bias in meta-analysis detected by a simple, graphical test.BMJ1997315629-34pmid:9310563
Egger M, Davey Smith G, Schneider M, Minder C. Bias in meta-analysis detected by a simple, graphical test. BMJ. 1997;315:629-34. [PMID: 9310563]

Abstract/FREE Full Text

[151] EggerM,

[152] Davey SmithG,

[153] SchneiderM,

[154] MinderC

[155] 32.↵

BlakeGJ,

RifaiN,

BuringJE,

RidkerPM

Blood pressure, C-reactive protein, and risk of future cardiovascular events.Circulation20031082993-9pmid:14638538
Blake GJ, Rifai N, Buring JE, Ridker PM. Blood pressure, C-reactive protein, and risk of future cardiovascular events. Circulation. 2003;108:2993-9. [PMID: 14638538]

Abstract/FREE Full Text

[156] BlakeGJ,

[157] RifaiN,

[158] BuringJE,

[159] RidkerPM

[160] 33.↵

KoenigW,

LöwelH,

BaumertJ,

MeisingerC

C-reactive protein modulates risk prediction based on the Framingham Score: implications for future risk assessment: results from a large cohort study in southern Germany.Circulation20041091349-53pmid:15023871
Koenig W, Löwel H, Baumert J, Meisinger C. C-reactive protein modulates risk prediction based on the Framingham Score: implications for future risk assessment: results from a large cohort study in southern Germany. Circulation. 2004;109:1349-53. [PMID: 15023871]

Abstract/FREE Full Text

[161] KoenigW,

[162] LöwelH,

[163] BaumertJ,

[164] MeisingerC

[165] 34.↵

KoenigW,

KhuseyinovaN,

LöwelH,

TrischlerG,

MeisingerC

Lipoprotein-associated phospholipase A2 adds to risk prediction of incident coronary events by C-reactive protein in apparently healthy middle-aged men from the general population: results from the 14-year follow-up of a large cohort from southern Germany.Circulation20041101903-8pmid:15451783
Koenig W, Khuseyinova N, Löwel H, Trischler G, Meisinger C. Lipoprotein-associated phospholipase A2 adds to risk prediction of incident coronary events by C-reactive protein in apparently healthy middle-aged men from the general population: results from the 14-year follow-up of a large cohort from southern Germany. Circulation. 2004;110:1903-8. [PMID: 15451783]

Abstract/FREE Full Text

[166] KoenigW,

[167] KhuseyinovaN,

[168] LöwelH,

[169] TrischlerG,

[170] MeisingerC

[171] 35.↵

LawlorDA,

SmithGD,

RumleyA,

LoweGD,

EbrahimS

Associations of fibrinogen and C-reactive protein with prevalent and incident coronary heart disease are attenuated by adjustment for confounding factors. British Women's Heart and Health Study.Thromb Haemost200593955-63pmid:15886815
Lawlor DA, Smith GD, Rumley A, Lowe GD, Ebrahim S. Associations of fibrinogen and C-reactive protein with prevalent and incident coronary heart disease are attenuated by adjustment for confounding factors. British Women's Heart and Health Study. Thromb Haemost. 2005;93:955-63. [PMID: 15886815]

Medline Web of Science

[172] LawlorDA,

[173] SmithGD,

[174] RumleyA,

[175] LoweGD,

[176] EbrahimS

[177] 36.↵

LoweGD,

YarnellJW,

RumleyA,

BaintonD,

SweetnamPM

C-reactive protein, fibrin D-dimer, and incident ischemic heart disease in the Speedwell study: are inflammation and fibrin turnover linked in pathogenesis?Arterioscler Thromb Vasc Biol200121603-10pmid:11304479
Lowe GD, Yarnell JW, Rumley A, Bainton D, Sweetnam PM. C-reactive protein, fibrin D-dimer, and incident ischemic heart disease in the Speedwell study: are inflammation and fibrin turnover linked in pathogenesis? Arterioscler Thromb Vasc Biol. 2001;21:603-10. [PMID: 11304479]

Abstract/FREE Full Text

[178] LoweGD,

[179] YarnellJW,

[180] RumleyA,

[181] BaintonD,

[182] SweetnamPM

[183] 37.↵

LoweGD,

SweetnamPM,

YarnellJW,

RumleyA,

RumleyC,

BaintonD

et al.C-reactive protein, fibrin d-dimer, and risk of ischemic heart disease: the Caerphilly and Speedwell studies.Arterioscler Thromb Vasc Biol2004241957-62pmid:15308549
Lowe GD, Sweetnam PM, Yarnell JW, Rumley A, Rumley C, Bainton D, et al. C-reactive protein, fibrin d-dimer, and risk of ischemic heart disease: the Caerphilly and Speedwell studies. Arterioscler Thromb Vasc Biol. 2004;24:1957-62. [PMID: 15308549]

Abstract/FREE Full Text

[184] LoweGD,

[185] SweetnamPM,

[186] YarnellJW,

[187] RumleyA,

[188] RumleyC,

[189] BaintonD

[190] 38.↵

PirroM,

BergeronJ,

DagenaisGR,

BernardPM,

CantinB,

DesprésJP

et al.Age and duration of follow-up as modulators of the risk for ischemic heart disease associated with high plasma C-reactive protein levels in men.Arch Intern Med20011612474-80pmid:11700160
Pirro M, Bergeron J, Dagenais GR, Bernard PM, Cantin B, Després JP, et al. Age and duration of follow-up as modulators of the risk for ischemic heart disease associated with high plasma C-reactive protein levels in men. Arch Intern Med. 2001;161:2474-80. [PMID: 11700160]

Abstract/FREE Full Text

[191] PirroM,

[192] BergeronJ,

[193] DagenaisGR,

[194] BernardPM,

[195] CantinB,

[196] DesprésJP

[197] 39.↵

RidkerPM,

RifaiN,

CookNR,

BradwinG,

BuringJE

Non-HDL cholesterol, apolipoproteins A-I and B100, standard lipid measures, lipid ratios, and CRP as risk factors for cardiovascular disease in women.JAMA2005294326-33pmid:16030277
Ridker PM, Rifai N, Cook NR, Bradwin G, Buring JE. Non-HDL cholesterol, apolipoproteins A-I and B100, standard lipid measures, lipid ratios, and CRP as risk factors for cardiovascular disease in women. JAMA. 2005;294:326-33. [PMID: 16030277]

Abstract/FREE Full Text

[198] RidkerPM,

[199] RifaiN,

[200] CookNR,

[201] BradwinG,

[202] BuringJE

[203] 40.↵

RidkerPM,

CookN

Clinical usefulness of very high and very low levels of C-reactive protein across the full range of Framingham Risk Scores.Circulation20041091955-9pmid:15051634
Ridker PM, Cook N. Clinical usefulness of very high and very low levels of C-reactive protein across the full range of Framingham Risk Scores. Circulation. 2004;109:1955-9. [PMID: 15051634]

Abstract/FREE Full Text

[204] RidkerPM,

[205] CookN

[206] 41.↵

RidkerPM,

RifaiN,

RoseL,

BuringJE,

CookNR

Comparison of C-reactive protein and low-density lipoprotein cholesterol levels in the prediction of first cardiovascular events.N Engl J Med20023471557-65pmid:12432042
Ridker PM, Rifai N, Rose L, Buring JE, Cook NR. Comparison of C-reactive protein and low-density lipoprotein cholesterol levels in the prediction of first cardiovascular events. N Engl J Med. 2002;347:1557-65. [PMID: 12432042]

Abstract/FREE Full Text

[207] RidkerPM,

[208] RifaiN,

[209] RoseL,

[210] BuringJE,

[211] CookNR

[212] 42.↵

St-PierreAC,

CantinB,

BergeronJ,

PirroM,

DagenaisGR,

DesprésJP

et al.Inflammatory markers and long-term risk of ischemic heart disease in men A 13-year follow-up of the Quebec Cardiovascular Study.Atherosclerosis2005182315-21pmid:16159604
St-Pierre AC, Cantin B, Bergeron J, Pirro M, Dagenais GR, Després JP, et al. Inflammatory markers and long-term risk of ischemic heart disease in men A 13-year follow-up of the Quebec Cardiovascular Study. Atherosclerosis. 2005;182:315-21. [PMID: 16159604]

CrossRef Medline Web of Science

[213] St-PierreAC,

[214] CantinB,

[215] BergeronJ,

[216] PirroM,

[217] DagenaisGR,

[218] DesprésJP

[219] 43.↵

WilsonPW,

NamBH,

PencinaM,

D'AgostinoRB, Sr,

BenjaminEJ,

O'DonnellCJ

C-reactive protein and risk of cardiovascular disease in men and women from the Framingham Heart Study.Arch Intern Med20051652473-8pmid:16314543
Wilson PW, Nam BH, Pencina M, D'Agostino RB Sr, Benjamin EJ, O'Donnell CJ. C-reactive protein and risk of cardiovascular disease in men and women from the Framingham Heart Study. Arch Intern Med. 2005;165:2473-8. [PMID: 16314543]

Abstract/FREE Full Text

[220] WilsonPW,

[221] NamBH,

[222] PencinaM,

[223] D'AgostinoRB, Sr,

[224] BenjaminEJ,

[225] O'DonnellCJ

[226] 44.↵

LucG,

BardJM,

Juhan-VagueI,

FerrieresJ,

EvansA,

AmouyelP

et al.PRIME Study GroupC-reactive protein, interleukin-6, and fibrinogen as predictors of coronary heart disease: the PRIME Study.Arterioscler Thromb Vasc Biol2003231255-61pmid:12775578
Luc G, Bard JM, Juhan-Vague I, Ferrieres J, Evans A, Amouyel P, et al; PRIME Study Group. C-reactive protein, interleukin-6, and fibrinogen as predictors of coronary heart disease: the PRIME Study. Arterioscler Thromb Vasc Biol. 2003;23:1255-61. [PMID: 12775578]

Abstract/FREE Full Text

[227] LucG,

[228] BardJM,

[229] Juhan-VagueI,

[230] FerrieresJ,

[231] EvansA,

[232] AmouyelP

[233] 45.↵

PaiJK,

PischonT,

MaJ,

MansonJE,

HankinsonSE,

JoshipuraK

et al.Inflammatory markers and the risk of coronary heart disease in men and women.N Engl J Med20043512599-610pmid:15602020
Pai JK, Pischon T, Ma J, Manson JE, Hankinson SE, Joshipura K, et al. Inflammatory markers and the risk of coronary heart disease in men and women. N Engl J Med. 2004;351:2599-610. [PMID: 15602020]

Abstract/FREE Full Text

[234] PaiJK,

[235] PischonT,

[236] MaJ,

[237] MansonJE,

[238] HankinsonSE,

[239] JoshipuraK

[240] 46.↵

PradhanAD,

MansonJE,

RossouwJE,

SiscovickDS,

MoutonCP,

RifaiN

et al.Inflammatory biomarkers, hormone replacement therapy, and incident coronary heart disease: prospective analysis from the Women's Health Initiative observational study.JAMA2002288980-7pmid:12190368
Pradhan AD, Manson JE, Rossouw JE, Siscovick DS, Mouton CP, Rifai N, et al. Inflammatory biomarkers, hormone replacement therapy, and incident coronary heart disease: prospective analysis from the Women's Health Initiative observational study. JAMA. 2002;288:980-7. [PMID: 12190368]

Abstract/FREE Full Text

[241] PradhanAD,

[242] MansonJE,

[243] RossouwJE,

[244] SiscovickDS,

[245] MoutonCP,

[246] RifaiN

[247] 47.↵

RidkerPM,

BuringJE,

ShihJ,

MatiasM,

HennekensCH

Prospective study of C-reactive protein and the risk of future cardiovascular events among apparently healthy women.Circulation199898731-3pmid:9727541
Ridker PM, Buring JE, Shih J, Matias M, Hennekens CH. Prospective study of C-reactive protein and the risk of future cardiovascular events among apparently healthy women. Circulation. 1998;98:731-3. [PMID: 9727541]

Abstract/FREE Full Text

[248] RidkerPM,

[249] BuringJE,

[250] ShihJ,

[251] MatiasM,

[252] HennekensCH

[253] 48.↵

RidkerPM,

CushmanM,

StampferMJ,

TracyRP,

HennekensCH

Inflammation, aspirin, and the risk of cardiovascular disease in apparently healthy men.N Engl J Med1997336973-9pmid:9077376
Ridker PM, Cushman M, Stampfer MJ, Tracy RP, Hennekens CH. Inflammation, aspirin, and the risk of cardiovascular disease in apparently healthy men. N Engl J Med. 1997;336:973-9. [PMID: 9077376]

Abstract/FREE Full Text

[254] RidkerPM,

[255] CushmanM,

[256] StampferMJ,

[257] TracyRP,

[258] HennekensCH

[259] 49.↵

RifaiN,

BuringJE,

LeeIM,

MansonJE,

RidkerPM

Is C-reactive protein specific for vascular disease in women?Ann Intern Med2002136529-33pmid:11926788
Rifai N, Buring JE, Lee IM, Manson JE, Ridker PM. Is C-reactive protein specific for vascular disease in women? Ann Intern Med. 2002;136:529-33. [PMID: 11926788]

Abstract/FREE Full Text

[260] RifaiN,

[261] BuringJE,

[262] LeeIM,

[263] MansonJE,

[264] RidkerPM

[265] 50.↵

van der MeerIM,

de MaatMP,

KiliaanAJ,

van der KuipDA,

HofmanA,

WittemanJC

The value of C-reactive protein in cardiovascular risk prediction: the Rotterdam Study.Arch Intern Med20031631323-8pmid:12796068
van der Meer IM, de Maat MP, Kiliaan AJ, van der Kuip DA, Hofman A, Witteman JC. The value of C-reactive protein in cardiovascular risk prediction: the Rotterdam Study. Arch Intern Med. 2003;163:1323-8. [PMID: 12796068]

Abstract/FREE Full Text

[266] van der MeerIM,

[267] de MaatMP,

[268] KiliaanAJ,

[269] van der KuipDA,

[270] HofmanA,

[271] WittemanJC

[272] 51.↵

WitherellHL,

SmithKL,

FriedmanGD,

LeyC,

ThomDH,

OrentreichN

et al.C-reactive protein, Helicobacter pylori, Chlamydia pneumoniae, cytomegalovirus and risk for myocardial infarction.Ann Epidemiol200313170-7pmid:12604160
Witherell HL, Smith KL, Friedman GD, Ley C, Thom DH, Orentreich N, et al. C-reactive protein, Helicobacter pylori, Chlamydia pneumoniae, cytomegalovirus and risk for myocardial infarction. Ann Epidemiol. 2003;13:170-7. [PMID: 12604160]

CrossRef Medline Web of Science

[273] WitherellHL,

[274] SmithKL,

[275] FriedmanGD,

[276] LeyC,

[277] ThomDH,

[278] OrentreichN

[279] 52.↵

BallantyneCM,

HoogeveenRC,

BangH,

CoreshJ,

FolsomAR,

HeissG

et al.Lipoprotein-associated phospholipase A2, high-sensitivity C-reactive protein, and risk for incident coronary heart disease in middle-aged men and women in the Atherosclerosis Risk in Communities (ARIC) study.Circulation2004109837-42pmid:14757686
Ballantyne CM, Hoogeveen RC, Bang H, Coresh J, Folsom AR, Heiss G, et al. Lipoprotein-associated phospholipase A2, high-sensitivity C-reactive protein, and risk for incident coronary heart disease in middle-aged men and women in the Atherosclerosis Risk in Communities (ARIC) study. Circulation. 2004;109:837-42. [PMID: 14757686]

Abstract/FREE Full Text

[280] BallantyneCM,

[281] HoogeveenRC,

[282] BangH,

[283] CoreshJ,

[284] FolsomAR,

[285] HeissG

[286] 53.↵

FolsomAR,

AleksicN,

CatellierD,

JunejaHS,

WuKK

C-reactive protein and incident coronary heart disease in the Atherosclerosis Risk In Communities (ARIC) study.Am Heart J2002144233-8pmid:12177639
Folsom AR, Aleksic N, Catellier D, Juneja HS, Wu KK. C-reactive protein and incident coronary heart disease in the Atherosclerosis Risk In Communities (ARIC) study. Am Heart J. 2002;144:233-8. [PMID: 12177639]

CrossRef Medline Web of Science

[287] FolsomAR,

[288] AleksicN,

[289] CatellierD,

[290] JunejaHS,

[291] WuKK

[292] 54.↵

GramJ,

BladbjergEM,

MøllerL,

SjølA,

JespersenJ

Tissue-type plasminogen activator and C-reactive protein in acute coronary heart disease. A nested case-control study.J Intern Med2000247205-12pmid:10692083
Gram J, Bladbjerg EM, Møller L, Sjøl A, Jespersen J. Tissue-type plasminogen activator and C-reactive protein in acute coronary heart disease. A nested case-control study. J Intern Med. 2000;247:205-12. [PMID: 10692083]

CrossRef Medline Web of Science

[293] GramJ,

[294] BladbjergEM,

[295] MøllerL,

[296] SjølA,

[297] JespersenJ

[298] 55.↵

BoekholdtSM,

HackCE,

SandhuMS,

LubenR,

BinghamSA,

WarehamNJ

et al.C-reactive protein levels and coronary artery disease incidence and mortality in apparently healthy men and women: the EPIC-Norfolk prospective population study 1993-2003.Atherosclerosis2006187415-22pmid:16257408
Boekholdt SM, Hack CE, Sandhu MS, Luben R, Bingham SA, Wareham NJ, et al. C-reactive protein levels and coronary artery disease incidence and mortality in apparently healthy men and women: the EPIC-Norfolk prospective population study 1993-2003. Atherosclerosis. 2006;187:415-22. [PMID: 16257408]

CrossRef Medline Web of Science

[299] BoekholdtSM,

[300] HackCE,

[301] SandhuMS,

[302] LubenR,

[303] BinghamSA,

[304] WarehamNJ

[305] 56.↵

CushmanM,

ArnoldAM,

PsatyBM,

ManolioTA,

KullerLH,

BurkeGL

et al.C-reactive protein and the 10-year incidence of coronary heart disease in older men and women: the cardiovascular health study.Circulation200511225-31pmid:15983251
Cushman M, Arnold AM, Psaty BM, Manolio TA, Kuller LH, Burke GL, et al. C-reactive protein and the 10-year incidence of coronary heart disease in older men and women: the cardiovascular health study. Circulation. 2005;112:25-31. [PMID: 15983251]

Abstract/FREE Full Text

[306] CushmanM,

[307] ArnoldAM,

[308] PsatyBM,

[309] ManolioTA,

[310] KullerLH,

[311] BurkeGL

[312] 57.↵

EverettBM,

KurthT,

BuringJE,

RidkerPM

The relative strength of C-reactive protein and lipid levels as determinants of ischemic stroke compared with coronary heart disease in women.J Am Coll Cardiol2006482235-42pmid:17161253
Everett BM, Kurth T, Buring JE, Ridker PM. The relative strength of C-reactive protein and lipid levels as determinants of ischemic stroke compared with coronary heart disease in women. J Am Coll Cardiol. 2006;48:2235-42. [PMID: 17161253]

Abstract/FREE Full Text

[313] EverettBM,

[314] KurthT,

[315] BuringJE,

[316] RidkerPM

[317] 58.↵

FolsomAR,

ChamblessLE,

BallantyneCM,

CoreshJ,

HeissG,

WuKK

et al.An assessment of incremental coronary risk prediction using C-reactive protein and other novel risk markers: the atherosclerosis risk in communities study.Arch Intern Med20061661368-73pmid:16832001
Folsom AR, Chambless LE, Ballantyne CM, Coresh J, Heiss G, Wu KK, et al. An assessment of incremental coronary risk prediction using C-reactive protein and other novel risk markers: the atherosclerosis risk in communities study. Arch Intern Med. 2006;166:1368-73. [PMID: 16832001]

Abstract/FREE Full Text

[318] FolsomAR,

[319] ChamblessLE,

[320] BallantyneCM,

[321] CoreshJ,

[322] HeissG,

[323] WuKK

[324] 59.↵

KoenigW,

KhuseyinovaN,

BaumertJ,

ThorandB,

LoewelH,

ChamblessL

et al.Increased concentrations of C-reactive protein and IL-6 but not IL-18 are independently associated with incident coronary events in middle-aged men and women: results from the MONICA/KORA Augsburg case-cohort study, 1984-2002.Arterioscler Thromb Vasc Biol2006262745-51pmid:17008587
Koenig W, Khuseyinova N, Baumert J, Thorand B, Loewel H, Chambless L, et al. Increased concentrations of C-reactive protein and IL-6 but not IL-18 are independently associated with incident coronary events in middle-aged men and women: results from the MONICA/KORA Augsburg case-cohort study, 1984-2002. Arterioscler Thromb Vasc Biol. 2006;26:2745-51. [PMID: 17008587]

Abstract/FREE Full Text

[325] KoenigW,

[326] KhuseyinovaN,

[327] BaumertJ,

[328] ThorandB,

[329] LoewelH,

[330] ChamblessL

[331] 60.↵

MoraS,

RifaiN,

BuringJE,

RidkerPM

Additive value of immunoassay-measured fibrinogen and high-sensitivity C-reactive protein levels for predicting incident cardiovascular events.Circulation2006114381-7pmid:16864722
Mora S, Rifai N, Buring JE, Ridker PM. Additive value of immunoassay-measured fibrinogen and high-sensitivity C-reactive protein levels for predicting incident cardiovascular events. Circulation. 2006;114:381-7. [PMID: 16864722]

Abstract/FREE Full Text

[332] MoraS,

[333] RifaiN,

[334] BuringJE,

[335] RidkerPM

[336] 61.↵

PischonT,

MöhligM,

HoffmannK,

SprangerJ,

WeikertC,

WillichSN

et al.Comparison of relative and attributable risk of myocardial infarction and stroke according to C-reactive protein and low-density lipoprotein cholesterol levels.Eur J Epidemiol200722429-38pmid:17557140
Pischon T, Möhlig M, Hoffmann K, Spranger J, Weikert C, Willich SN, et al. Comparison of relative and attributable risk of myocardial infarction and stroke according to C-reactive protein and low-density lipoprotein cholesterol levels. Eur J Epidemiol. 2007;22:429-38. [PMID: 17557140]

CrossRef Medline

[337] PischonT,

[338] MöhligM,

[339] HoffmannK,

[340] SprangerJ,

[341] WeikertC,

[342] WillichSN

[343] 62.↵

TuomistoK,

JousilahtiP,

SundvallJ,

PajunenP,

SalomaaV

C-reactive protein, interleukin-6 and tumor necrosis factor alpha as predictors of incident coronary and cardiovascular events and total mortality. A population-based, prospective study.Thromb Haemost200695511-8pmid:16525580
Tuomisto K, Jousilahti P, Sundvall J, Pajunen P, Salomaa V. C-reactive protein, interleukin-6 and tumor necrosis factor alpha as predictors of incident coronary and cardiovascular events and total mortality. A population-based, prospective study. Thromb Haemost. 2006;95:511-8. [PMID: 16525580]

Medline Web of Science

[344] TuomistoK,

[345] JousilahtiP,

[346] SundvallJ,

[347] PajunenP,

[348] SalomaaV

[349] 63.↵

TzoulakiI,

MurrayGD,

LeeAJ,

RumleyA,

LoweGD,

FowkesFG

Relative value of inflammatory, hemostatic, and rheological factors for incident myocardial infarction and stroke: the Edinburgh Artery Study.Circulation20071152119-27pmid:17404162
Tzoulaki I, Murray GD, Lee AJ, Rumley A, Lowe GD, Fowkes FG. Relative value of inflammatory, hemostatic, and rheological factors for incident myocardial infarction and stroke: the Edinburgh Artery Study. Circulation. 2007;115:2119-27. [PMID: 17404162]

Abstract/FREE Full Text

[350] TzoulakiI,

[351] MurrayGD,

[352] LeeAJ,

[353] RumleyA,

[354] LoweGD,

[355] FowkesFG

[356] 64.↵

KullerLH,

TracyRP,

ShatenJ,

MeilahnEN

Relation of C-reactive protein and coronary heart disease in the MRFIT nested case-control study. Multiple Risk Factor Intervention Trial.Am J Epidemiol1996144537-47pmid:8797513
Kuller LH, Tracy RP, Shaten J, Meilahn EN. Relation of C-reactive protein and coronary heart disease in the MRFIT nested case-control study. Multiple Risk Factor Intervention Trial. Am J Epidemiol. 1996;144:537-47. [PMID: 8797513]

Abstract/FREE Full Text

[357] KullerLH,

[358] TracyRP,

[359] ShatenJ,

[360] MeilahnEN

[361] 65.↵

AgewallS,

WikstrandJ,

FagerbergB

Prothrombin fragment 1 + 2 is a risk factor for myocardial infarction in treated hypertensive men.J Hypertens199816537-41pmid:9797200
Agewall S, Wikstrand J, Fagerberg B. Prothrombin fragment 1 + 2 is a risk factor for myocardial infarction in treated hypertensive men. J Hypertens. 1998;16:537-41. [PMID: 9797200]

CrossRef Medline Web of Science

[362] AgewallS,

[363] WikstrandJ,

[364] FagerbergB

[365] 66.↵

RoivainenM,

Viik-KajanderM,

PalosuoT,

ToivanenP,

LeinonenM,

SaikkuP

et al.Infections, inflammation, and the risk of coronary heart disease.Circulation2000101252-7pmid:10645920
Roivainen M, Viik-Kajander M, Palosuo T, Toivanen P, Leinonen M, Saikku P, et al. Infections, inflammation, and the risk of coronary heart disease. Circulation. 2000;101:252-7. [PMID: 10645920]

Abstract/FREE Full Text

[366] RoivainenM,

[367] Viik-KajanderM,

[368] PalosuoT,

[369] ToivanenP,

[370] LeinonenM,

[371] SaikkuP

[372] 67.↵

StrandbergTE,

TilvisRS

C-reactive protein, cardiovascular risk factors, and mortality in a prospective study in the elderly.Arterioscler Thromb Vasc Biol2000201057-60pmid:10764673
Strandberg TE, Tilvis RS. C-reactive protein, cardiovascular risk factors, and mortality in a prospective study in the elderly. Arterioscler Thromb Vasc Biol. 2000;20:1057-60. [PMID: 10764673]

Abstract/FREE Full Text

[373] StrandbergTE,

[374] TilvisRS

[375] 68.↵

PackardCJ,

O'ReillyDS,

CaslakeMJ,

McMahonAD,

FordI,

CooneyJ

et al.Lipoprotein-associated phospholipase A2 as an independent predictor of coronary heart disease. West of Scotland Coronary Prevention Study Group.N Engl J Med20003431148-55pmid:11036120
Packard CJ, O'Reilly DS, Caslake MJ, McMahon AD, Ford I, Cooney J, et al. Lipoprotein-associated phospholipase A2 as an independent predictor of coronary heart disease. West of Scotland Coronary Prevention Study Group. N Engl J Med. 2000;343:1148-55. [PMID: 11036120]

Abstract/FREE Full Text

[376] PackardCJ,

[377] O'ReillyDS,

[378] CaslakeMJ,

[379] McMahonAD,

[380] FordI,

[381] CooneyJ

[382] 69.↵

RidkerPM

High-sensitivity C-reactive protein: potential adjunct for global risk assessment in the primary prevention of cardiovascular disease.Circulation20011031813-8pmid:11282915
Ridker PM. High-sensitivity C-reactive protein: potential adjunct for global risk assessment in the primary prevention of cardiovascular disease. Circulation. 2001;103:1813-8. [PMID: 11282915]

Abstract/FREE Full Text

[383] RidkerPM

[384] 70.↵

HarrisTB,

FerrucciL,

TracyRP,

CortiMC,

WacholderS,

EttingerWH, Jr

et al.Associations of elevated interleukin-6 and C-reactive protein levels with mortality in the elderly.Am J Med1999106506-12pmid:10335721
Harris TB, Ferrucci L, Tracy RP, Corti MC, Wacholder S, Ettinger WH Jr, et al. Associations of elevated interleukin-6 and C-reactive protein levels with mortality in the elderly. Am J Med. 1999;106:506-12. [PMID: 10335721]

CrossRef Medline Web of Science

[385] HarrisTB,

[386] FerrucciL,

[387] TracyRP,

[388] CortiMC,

[389] WacholderS,

[390] EttingerWH, Jr

[391] 71.↵

JagerA,

van HinsberghVW,

KostensePJ,

EmeisJJ,

YudkinJS,

NijpelsG

et al.von Willebrand factor, C-reactive protein, and 5-year mortality in diabetic and nondiabetic subjects: the Hoorn Study.Arterioscler Thromb Vasc Biol1999193071-8pmid:10591689
Jager A, van Hinsbergh VW, Kostense PJ, Emeis JJ, Yudkin JS, Nijpels G, et al. von Willebrand factor, C-reactive protein, and 5-year mortality in diabetic and nondiabetic subjects: the Hoorn Study. Arterioscler Thromb Vasc Biol. 1999;19:3071-8. [PMID: 10591689]

Abstract/FREE Full Text

[392] JagerA,

[393] van HinsberghVW,

[394] KostensePJ,

[395] EmeisJJ,

[396] YudkinJS,

[397] NijpelsG

[398] 72.↵

CookNR

Use and misuse of the receiver operating characteristic curve in risk prediction.Circulation2007115928-35pmid:17309939
Cook NR. Use and misuse of the receiver operating characteristic curve in risk prediction. Circulation. 2007;115:928-35. [PMID: 17309939]

Abstract/FREE Full Text

[399] CookNR

[400] 73.↵

GreenlandP,

O'MalleyPG

When is a new prediction marker useful? A consideration of lipoprotein-associated phospholipase A2 and C-reactive protein for stroke risk [Editorial].Arch Intern Med20051652454-6pmid:16314539
Greenland P, O'Malley PG. When is a new prediction marker useful? A consideration of lipoprotein-associated phospholipase A2 and C-reactive protein for stroke risk [Editorial]. Arch Intern Med. 2005;165:2454-6. [PMID: 16314539]

FREE Full Text

[401] GreenlandP,

[402] O'MalleyPG

[403] 74.↵

Lloyd-JonesDM,

LiuK,

TianL,

GreenlandP

Narrative review: Assessment of C-reactive protein in risk prediction for cardiovascular disease.Ann Intern Med200614535-42pmid:16818927
Lloyd-Jones DM, Liu K, Tian L, Greenland P. Narrative review: Assessment of C-reactive protein in risk prediction for cardiovascular disease. Ann Intern Med. 2006;145:35-42. [PMID: 16818927]

Abstract/FREE Full Text

[404] Lloyd-JonesDM,

[405] LiuK,

[406] TianL,

[407] GreenlandP

[408] 75.↵

KoenigW

Cardiovascular biomarkers: added value with an integrated approach? [Editorial].Circulation20071163-5pmid:17606853
Koenig W. Cardiovascular biomarkers: added value with an integrated approach? [Editorial]. Circulation. 2007;116:3-5. [PMID: 17606853]

FREE Full Text

[409] KoenigW

[410] 76.↵

PepeMS,

JanesH,

LongtonG,

LeisenringW,

NewcombP

Limitations of the odds ratio in gauging the performance of a diagnostic, prognostic, or screening marker.Am J Epidemiol2004159882-90pmid:15105181
Pepe MS, Janes H, Longton G, Leisenring W, Newcomb P. Limitations of the odds ratio in gauging the performance of a diagnostic, prognostic, or screening marker. Am J Epidemiol. 2004;159:882-90. [PMID: 15105181]

Abstract/FREE Full Text

[411] PepeMS,

[412] JanesH,

[413] LongtonG,

[414] LeisenringW,

[415] NewcombP

[416] 77.↵

MoonsKG,

HarrellFE

Sensitivity and specificity should be de-emphasized in diagnostic accuracy studies.Acad Radiol200310670-2pmid:12809422
Moons KG, Harrell FE. Sensitivity and specificity should be de-emphasized in diagnostic accuracy studies. Acad Radiol. 2003;10:670-2. [PMID: 12809422]

CrossRef Medline Web of Science

[417] MoonsKG,

[418] HarrellFE

[419] 78.↵

PepeMS,

FengZ,

HuangY,

LongtonG,

PrenticeR,

ThompsonIM

et al.Integrating the predictiveness of a marker with its performance as a classifier.Am J Epidemiol2008167362-8pmid:17982157
Pepe MS, Feng Z, Huang Y, Longton G, Prentice R, Thompson IM, et al. Integrating the predictiveness of a marker with its performance as a classifier. Am J Epidemiol. 2008;167:362-8. [PMID: 17982157]

Abstract/FREE Full Text

[420] PepeMS,

[421] FengZ,

[422] HuangY,

[423] LongtonG,

[424] PrenticeR,

[425] ThompsonIM

[426] 79.↵

WilsonPWF,

PencinaMJ,

JacquesP,

SelhubJ,

D'AgostinoRB,

O'DonnellCJ

C-reactive protein and reclassification of cardiovascular risk in the Framingham Heart Study.Circ Cardiovasc Qual Outcomes2008192-97
Wilson PWF, Pencina MJ, Jacques P, Selhub J, D'Agostino RB, O'Donnell CJ. C-reactive protein and reclassification of cardiovascular risk in the Framingham Heart Study. Circ Cardiovasc Qual Outcomes. 2008;1:92-97.

[427] WilsonPWF,

[428] PencinaMJ,

[429] JacquesP,

[430] SelhubJ,

[431] D'AgostinoRB,

[432] O'DonnellCJ

[433] 80.↵

National Cholesterol Education Program (NCEP) Expert Panel on Detection, Evaluation, and Treatment of High Blood Cholesterol in Adults (Adult Treatment Panel III)Third Report of the National Cholesterol Education Program (NCEP) Expert Panel on Detection, Evaluation, and Treatment of High Blood Cholesterol in Adults (Adult Treatment Panel III) final report.Circulation20021063143-421pmid:12485966
National Cholesterol Education Program (NCEP) Expert Panel on Detection, Evaluation, and Treatment of High Blood Cholesterol in Adults (Adult Treatment Panel III). Third Report of the National Cholesterol Education Program (NCEP) Expert Panel on Detection, Evaluation, and Treatment of High Blood Cholesterol in Adults (Adult Treatment Panel III) final report. Circulation. 2002;106:3143-421. [PMID: 12485966]

FREE Full Text

[434] 81.↵

AjaniUA,

FordES,

MokdadAH

Prevalence of high C-reactive protein in persons with serum lipid concentrations within recommended values.Clin Chem2004501618-22pmid:15205370
Ajani UA, Ford ES, Mokdad AH. Prevalence of high C-reactive protein in persons with serum lipid concentrations within recommended values. Clin Chem. 2004;50:1618-22. [PMID: 15205370]

Abstract/FREE Full Text

[435] AjaniUA,

[436] FordES,

[437] MokdadAH

[438] 82.↵

HutchinsonWL,

KoenigW,

FröhlichM,

SundM,

LoweGD,

PepysMB

Immunoradiometric assay of circulating C-reactive protein: age-related values in the adult general population.Clin Chem200046934-8pmid:10894836
Hutchinson WL, Koenig W, Fröhlich M, Sund M, Lowe GD, Pepys MB. Immunoradiometric assay of circulating C-reactive protein: age-related values in the adult general population. Clin Chem. 2000;46:934-8. [PMID: 10894836]

Abstract/FREE Full Text

[439] HutchinsonWL,

[440] KoenigW,

[441] FröhlichM,

[442] SundM,

[443] LoweGD,

[444] PepysMB

[445] 83.↵

WilkinsJ,

GallimoreJR,

MooreEG,

PepysMB

Rapid automated high sensitivity enzyme immunoassay of C-reactive protein.Clin Chem1998441358-61pmid:9625071
Wilkins J, Gallimore JR, Moore EG, Pepys MB. Rapid automated high sensitivity enzyme immunoassay of C-reactive protein. Clin Chem. 1998;44:1358-61. [PMID: 9625071]

FREE Full Text

[446] WilkinsJ,

[447] GallimoreJR,

[448] MooreEG,

[449] PepysMB

[450] 84.↵

KoenigW,

SundM,

FröhlichM,

LöwelH,

HutchinsonWL,

PepysMB

Refinement of the association of serum C-reactive protein concentration and coronary heart disease risk by correction for within-subject variation over time: the MONICA Augsburg studies, 1984 and 1987.Am J Epidemiol2003158357-64pmid:12915501
Koenig W, Sund M, Fröhlich M, Löwel H, Hutchinson WL, Pepys MB. Refinement of the association of serum C-reactive protein concentration and coronary heart disease risk by correction for within-subject variation over time: the MONICA Augsburg studies, 1984 and 1987. Am J Epidemiol. 2003;158:357-64. [PMID: 12915501]

Abstract/FREE Full Text

[451] KoenigW,

[452] SundM,

[453] FröhlichM,

[454] LöwelH,

[455] HutchinsonWL,

[456] PepysMB

[457] 85.↵

OckeneIS,

MatthewsCE,

RifaiN,

RidkerPM,

ReedG,

StanekE

Variability and classification accuracy of serial high-sensitivity C-reactive protein measurements in healthy adults.Clin Chem200147444-50pmid:11238295
Ockene IS, Matthews CE, Rifai N, Ridker PM, Reed G, Stanek E. Variability and classification accuracy of serial high-sensitivity C-reactive protein measurements in healthy adults. Clin Chem. 2001;47:444-50. [PMID: 11238295]

Abstract/FREE Full Text

[458] OckeneIS,

[459] MatthewsCE,

[460] RifaiN,

[461] RidkerPM,

[462] ReedG,

[463] StanekE

[464] 86.↵

NicklasBJ,

YouT,

PahorM

Behavioural treatments for chronic systemic inflammation: effects of dietary weight loss and exercise training.CMAJ20051721199-209pmid:15851714
Nicklas BJ, You T, Pahor M. Behavioural treatments for chronic systemic inflammation: effects of dietary weight loss and exercise training. CMAJ. 2005;172:1199-209. [PMID: 15851714]

Abstract/FREE Full Text

[465] NicklasBJ,

[466] YouT,

[467] PahorM

[468] 87.↵

NissenSE,

TuzcuEM,

SchoenhagenP,

CroweT,

SasielaWJ,

TsaiJ

et al.Reversal of Atherosclerosis with Aggressive Lipid Lowering (REVERSAL) InvestigatorsStatin therapy, LDL cholesterol, C-reactive protein, and coronary artery disease.N Engl J Med200535229-38pmid:15635110
Nissen SE, Tuzcu EM, Schoenhagen P, Crowe T, Sasiela WJ, Tsai J, et al; Reversal of Atherosclerosis with Aggressive Lipid Lowering (REVERSAL) Investigators. Statin therapy, LDL cholesterol, C-reactive protein, and coronary artery disease. N Engl J Med. 2005;352:29-38. [PMID: 15635110]

Abstract/FREE Full Text

[469] NissenSE,

[470] TuzcuEM,

[471] SchoenhagenP,

[472] CroweT,

[473] SasielaWJ,

[474] TsaiJ

[475] 88.↵

RidkerPM,

CannonCP,

MorrowD,

RifaiN,

RoseLM,

McCabeCH

et al.Pravastatin or Atorvastatin Evaluation and Infection Therapy-Thrombolysis in Myocardial Infarction 22 (PROVE IT-TIMI 22) InvestigatorsC-reactive protein levels and outcomes after statin therapy.N Engl J Med200535220-8pmid:15635109
Ridker PM, Cannon CP, Morrow D, Rifai N, Rose LM, McCabe CH, et al; Pravastatin or Atorvastatin Evaluation and Infection Therapy-Thrombolysis in Myocardial Infarction 22 (PROVE IT-TIMI 22) Investigators. C-reactive protein levels and outcomes after statin therapy. N Engl J Med. 2005;352:20-8. [PMID: 15635109]

Abstract/FREE Full Text

[476] RidkerPM,

[477] CannonCP,

[478] MorrowD,

[479] RifaiN,

[480] RoseLM,

[481] McCabeCH

[482] 89.↵

RidkerPM,

DanielsonE,

FonsecaFA,

GenestJ,

GottoAM, Jr,

KasteleinJJ

et al.JUPITER Study GroupRosuvastatin to prevent vascular events in men and women with elevated C-reactive protein.N Engl J Med20083592195-207pmid:18997196
Ridker PM, Danielson E, Fonseca FA, Genest J, Gotto AM Jr, Kastelein JJ, et al; JUPITER Study Group. Rosuvastatin to prevent vascular events in men and women with elevated C-reactive protein. N Engl J Med. 2008;359:2195-207. [PMID: 18997196]

Abstract/FREE Full Text

[483] RidkerPM,

[484] DanielsonE,

[485] FonsecaFA,

[486] GenestJ,

[487] GottoAM, Jr,

[488] KasteleinJJ

[489] 90.↵

HlatkyMA

Expanding the orbit of primary prevention—moving beyond JUPITER [Editorial].N Engl J Med20083592280-2pmid:18997195
Hlatky MA. Expanding the orbit of primary prevention—moving beyond JUPITER [Editorial]. N Engl J Med. 2008;359:2280-2. [PMID: 18997195]

FREE Full Text

[490] HlatkyMA

[491] 91.↵

AlbertMA,

GlynnRJ,

RidkerPM

Plasma concentration of C-reactive protein and the calculated Framingham Coronary Heart Disease Risk Score.Circulation2003108161-5pmid:12835213
Albert MA, Glynn RJ, Ridker PM. Plasma concentration of C-reactive protein and the calculated Framingham Coronary Heart Disease Risk Score. Circulation. 2003;108:161-5. [PMID: 12835213]

Abstract/FREE Full Text

[492] AlbertMA,

[493] GlynnRJ,

[494] RidkerPM

[495] 92.↵

BermudezEA,

RifaiN,

BuringJ,

MansonJE,

RidkerPM

Interrelationships among circulating interleukin-6, C-reactive protein, and traditional cardiovascular risk factors in women.Arterioscler Thromb Vasc Biol2002221668-73pmid:12377747
Bermudez EA, Rifai N, Buring J, Manson JE, Ridker PM. Interrelationships among circulating interleukin-6, C-reactive protein, and traditional cardiovascular risk factors in women. Arterioscler Thromb Vasc Biol. 2002;22:1668-73. [PMID: 12377747]

Abstract/FREE Full Text

[496] BermudezEA,

[497] RifaiN,

[498] BuringJ,

[499] MansonJE,

[500] RidkerPM

[501] 93.↵

Engström G. The role of inflammation for heart disease risk cannot be determined by correlations between C-reactive protein and risk factors [Letter]. Arch Intern Med. 2006;166:1040; author reply 1040-1. [PMID: 16682580]

C-Reactive Protein as a Risk Factor for Coronary Heart Disease: A Systematic Review and Meta-analyses for the U.S. Preventive Services Task Force

Abstract

Methods

Data Sources and Searches

Study Selection

Data Extraction and Quality Assessment

Data Synthesis and Analysis

Role of the Funding Source

Results

Study Characteristics

Meta-analysis of Fair-Quality or Better Studies

Meta-analysis of Good-Quality Studies

Reclassification of Persons at Intermediate Risk

Discussion

Article and Author Information

References

Responses to this article

Summary for Patients

This Article

Services

Rapid Responses

Citing Articles

Google Scholar

PubMed

Related Content

Social Bookmarking

Navigate This Article

Current Issue

Features

Info for Users

Annals in the News

Most Read

Clinical Trials

Classifieds

C-Reactive Protein as a Risk Factor for Coronary Heart Disease: A Systematic Review and Meta-analyses for the U.S. Preventive Services Task Force

Abstract

Methods

Data Sources and Searches

Study Selection

Data Extraction and Quality Assessment

Data Synthesis and Analysis

Role of the Funding Source

Results

Study Characteristics

Meta-analysis of Fair-Quality or Better Studies

Meta-analysis of Good-Quality Studies

Reclassification of Persons at Intermediate Risk

Discussion

Article and Author Information

References

Related articles

Responses to this article

Summary for Patients

This Article

Services

Rapid Responses

Citing Articles

Google Scholar

PubMed

Related Content

Social Bookmarking

Navigate This Article

Current Issue

Features

Info for Users

Annals in the News

Most Read

Clinical Trials

Classifieds