Prospective Evaluation of Risk Factors for Bloodstream Infection in Patients Receiving Home Infusion Therapy

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	Tokars, J. I.

	Jarvis, W. R.

ARTICLE

Prospective Evaluation of Risk Factors for Bloodstream Infection in Patients Receiving Home Infusion Therapy

Jerome I. Tokars, MD, MPH; Susan T. Cookson, MD; Margaret A. McArthur, RN; Cindy L. Boyer, RN, MSN; Allison J. McGeer, MSc, MD, FRCPC; and William R. Jarvis, MD

7 September 1999 | Volume 131 Issue 5 | Pages 340-347

Background: Intravenous therapy in the outpatient and homesettings is commonplace for many diseases and nutritional disorders.Few data are available on the rate of and risk factors for bloodstreaminfection among patients receiving such therapy.

Objective: To determine rates of and risk factors for bloodstreaminfection among patients receiving home infusion therapy.

Design: Prospective, observational cohort study.

Setting: Cleveland, Ohio, and Toronto, Ontario, Canada.

Patients: Patients receiving home infusion therapy througha central or midline catheter.

Measurements: Primary laboratory-confirmed bloodstream infection.

Results: Among 827 patients (988 catheters), the most commondiagnoses were infections other than HIV (67%), cancer (24%),nutritional and digestive disease (17%), heart disease (14%),receipt of bone marrow or solid organ transplants (11%), andHIV infection (7%). Sixty-nine bloodstream infections occurredduring 69 532 catheter-days (0.99 infections per 1000 days).In a Cox regression model with time-dependent covariates, independentrisk factors for bloodstream infection were recent receipt ofa bone marrow transplant (hazard ratio, 5.8 [95% CI, 3.0 to11.3]), receipt of total parenteral nutrition (hazard ratio,4.1 [CI, 2.3 to 7.2]), receipt of therapy outside the home (forexample, in an outpatient clinic or physician's office) (hazardratio, 3.6 [CI, 2.2 to 5.9]), use of a multilumen catheter (hazardratio, 2.8 [CI, 1.7 to 4.7]), and previous bloodstream infection(hazard ratio, 2.5 [CI, 1.5 to 4.2]). Rates of bloodstream infectionper 1000 catheter-days varied from 0.16 for patients with noneof these 5 risk factors to 6.77 for patients with 3 or morerisk factors. Centrally inserted venous catheters were associatedwith a higher risk than implanted ports were, but the differencewas not statistically significant.

Conclusion: Bloodstream infections seem to be infrequent amongoutpatients receiving infusions through central and midlinecatheters. However, the rate of infection increases with bonemarrow transplantation, parenteral nutrition, infusion therapyin a hospital clinic or physician's office, and use of multilumencatheters. Compared with implanted ports or peripherally insertedcatheters, centrally inserted venous catheters may confer greaterrisk for bloodstream infection.

Expenditures are growing rapidly for health care delivered inthe home (1, 2), which often includes intravenous therapy. Althoughintravenous infusion may cause bloodstream infection, few prospectivestudies have assessed the risk for this infection in the homesetting. Needleless infusion devices have been introduced inthe hospital and home settings as a way to prevent needlestickinjuries. These devices connect the catheter with the infusiontubing, allowing fluids to be administered without the use ofa needle. Several investigations among patients receiving homeinfusion therapy from 1993 to 1995 showed an association betweenbloodstream infection and needleless devices under certain circumstances(3-7). The investigations were limited: They were retrospective,and some data were not available.

We report results of a prospective study of bloodstream infectionamong patients receiving home infusion therapy. We sought todetermine rates of and risk factors for bloodstream infectionand to evaluate the importance of needleless devices and otherrisk factors identified in the investigations cited above.

Methods

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Patients

Patients were enrolled at two study sites, one in Toronto, Ontario,Canada, and one in Cleveland, Ohio. The study protocol was approvedby the institutional review boards at the Centers for DiseaseControl and Prevention and at all institutions involved at thetwo study sites. At the Toronto site, eligible patients includedall patients referred to one of five home infusion agencies(which provide approximately 90% of infusion therapy in thisregion) from any Toronto-area hospital, patients in the TorontoHospital total parenteral nutrition program, and patients inthe Princess Margaret Hospital oncology program. At the Clevelandsite, eligible patients included all patients at four hospitals,including The Cleveland Clinic Foundation Hospital, who receivedinfusion therapy from the home infusion agency affiliated withThe Cleveland Clinic Foundation. At each site, patients werefirst asked for verbal consent to participate. Patients whogranted this consent were interviewed by a study nurse and wereasked to provide written informed consent (in Toronto) or weremailed forms for written consent (in Cleveland).

Design

This prospective cohort study was performed from 1 April 1996to 30 April 1997 in Toronto and from 1 May 1996 to 30 May 1997in Cleveland. For all eligible patients, an anonymous pre-enrollmentform without personal identifiers was completed; for patientswho consented and were enrolled, additional forms were completed(Table 1). Data for completion of all forms were obtained fromthe hospital records and infusion agency records and by interviewingpatients. Multiple sources were often used, especially to checkinformation provided by patients. On-site study nurses completedall forms and entered information into computer databases. Patientswere seen at frequencies ranging from two to three times perday to once per month, depending on diagnosis and indicationsfor therapy.

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Table 1. Data Collection Forms and Potential Risk Factors Studied

An infection form was completed for episodes of suspected infection[Table 1]. Bloodstream infection was diagnosed if all of thefollowing features were present: 1) one or more positive bloodcultures, 2) antimicrobial therapy or catheter removal, and3) no infection at another site that could have caused the bacteremia.For low-virulence organisms, such as coagulase-negative staphylococci,we required the additional criteria of one or more clinicalfeatures (fever, chills, or purulent exudate at the catheterinsertion site) and at least two positive blood cultures. Episodesthat occurred within 2 days of enrollment or hospital dischargewere excluded because they would not represent home health care-relatedinfections.

Statistical Analysis

Data from the catheter, infusion therapy, and infection-controlforms were collected and analyzed as time-dependent variables.For example, in a single patient, catheter type A might havebeen used for days 1 to 14; that catheter might then have beenremoved and catheter type B inserted and used for days 15 to45. For such variables, the unit of analysis is the patient,but the values of the variables are allowed to change at differenttimes of follow-up.

Patients were included in the study only during periods in whichthey had a central or midline catheter at home; therefore, thenumber of days that a patient was followed in the study equalsthe number of catheter-days. Patients whose catheters had beenplaced before the study started were included, but bloodstreaminfections in these patients were included only if they occurred30 or more days after enrollment, were associated with a differentcatheter, or were caused by an organism different from thatwhich had caused bloodstream infection before enrollment. Forpatients who had a bloodstream infection during the study, dataon patient-days and infections were excluded for 1 month afterthe infection and were included again thereafter; subsequentbloodstream infections were counted if the patient had a differentcatheter or if a different organism was isolated. Therefore,some patients had more than one bloodstream infection duringthe study.

By using SAS for Personal Computers (SAS Institute, Inc., Cary,North Carolina), the separate databases were merged into a commondatabase for analysis. Some of the time-dependent risk factorsmay have changed between the day of microbial invasion and theday on which positive blood cultures were obtained; to accountfor this effect, bloodstream infections were included in thecommon database as of 2 days before the date on which they werereported. Incidence density rates (bloodstream infection ratesper 1000 catheter-days) were calculated by dividing the numberof bloodstream infections by the number of catheter-days andmultiplying the result by 1000.

Univariable and multivariable analyses were performed by usingCox regression models for time-dependent covariates (8). Factorsthat were found to be statistically significant (P < 0.05)in univariable analysis were considered for inclusion in themultivariable model by using a forward stepwise algorithm. Independentlystatistically significant variables (P < 0.05)were included in the final multivariable model. Selected variablesthat were not independently significant were then individuallyinserted into the final regression model to determine hazardratios and CIs after adjustment for the factors in the finalmodel. We calculated 95% CIs for hazard ratios by subtractingfrom or adding to the variable estimate 1.96 times its SE andexponentiating the result. All reported P values are two-sided.

Role of the Funding Source

This study was funded by the U.S. federal government. No proprietaryinterest had a role in the collection, analysis, or interpretationof the data or in the decision to submit the paper for publication.

Results

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Enrollment

Of 1528 eligible patients, 827 (54%) were enrolled: 62% (354of 569) of eligible patients at the Toronto site and 49% (473of 959) of those at the Cleveland site. At the Toronto site,the primary reason given for nonenrollment was that patientswere overwhelmed by their illness and were not able to copewith anything else. At the Cleveland site, the lower enrollmentrate was attributed to the fact that patients were asked toprovide informed consent by mail rather than at a face-to-facemeeting. All diagnoses included on the pre-enrollment form werelisted more often for enrolled than nonenrolled patients; themost common diagnoses of enrolled patients were infections otherthan HIV (67%) and cancer (24%) (Table 2). Compared with nonenrolledpatients, enrolled patients were more likely to receive totalparenteral nutrition and less likely to receive chemotherapy.

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Table 2. Comparison of Patients Who Were Not Enrolled with Enrolled Patients

The 827 enrolled patients had 988 catheters. Of these, 433 (44%)were centrally inserted venous catheters, including 215 Hickmancatheters and 125 Cook catheters; 324 (33%) were peripherallyinserted central catheters, including 218 Per-Q-Cath catheters(Bard Access Systems, Murray Hill, New York); 155 (16%) weremidline catheters, including 96 Landmark catheters (Menlo Care,Inc., Menlo Park, California); and 76 (8%) were implanted ports,including 70 Port-A-Cath catheters (SIMS Deltec, Inc., St. Paul,Minnesota). The median follow-up time was 67 days for patientswith centrally inserted venous catheters, 27 days for thosewith peripherally inserted central catheters, 17 days for thosewith midline catheters, and 155 for those with implanted ports.Among the centrally inserted venous catheters, all were tunneledand cuffed, and none were impregnated with antiseptic agents.We recorded dates of insertion and removal of catheters butnot whether catheters were removed because of occlusion. Forthe 988 catheters, needle access was used in 108 (11%), needlelessaccess was used in 877 (89%), and protected needle access wasused in 3 (<1%). Of the needleless accesses, 792 (89%) wereInterlink systems (Baxter International, Deerfield, Illinois).

Bloodstream Infections

A total of 69 bloodstream infections occurred among 59 patients;50 patients had 1 bloodstream infection, 8 had 2 bloodstreaminfections, and 1 had 3 bloodstream infections. Among patientswith 2 or more bloodstream infections, the median duration betweeninfections was 119 days (range, 40 to 187 days). The blood specimenshowing bacteremia was taken from a peripheral vein in 34 infections(49%), the catheter in 21 infections (30%), and an unknown sitein 14 infections (20%). Symptoms included fever in 58 infections(84%), chills in 43 infections (62%), redness at the catheterinsertion site in 10 infections (14%), and purulence at thecatheter insertion site in 5 infections (7%). At the time ofinfection, the leukocyte count was 100 to 1000 cells x 10⁹/Lin 10.1% of patients and more than 10 000 cells x 10⁹/L in 23.2%(median leukocyte count, 5800 cells x 10⁹/L [range, 100 to 24700 cells x 10⁹/L]). Ten episodes of concomitant infection (7urine, 2 lung, and 1 other) occurred. The catheter was removedin 36 (52%) episodes of bloodstream infection, and intravenousantimicrobial therapy was begun in 68 (99%) episodes.

The 69 bloodstream infections included 14 (20%) that were polymicrobial(2 microorganisms were isolated for all episodes). The 83 isolatesconsisted of 48 (58%) gram-positive cocci, including 23 coagulase-negativestaphylococci, 8 Staphylococcus aureus, 6 enterococci, 5 corynebacteria,and 6 others; 27 (32%) gram-negative rods, including 7 Klebsiellaspecies, 5 Escherichia coli, 4 Acinetobacter species, 3 Enterobacterspecies, and 8 others; and 8 (10%) fungi, including 7 Candidaspecies.

Risk Factors for Bloodstream Infections

The 827 patients were followed for a total of 69 532 catheter-days(median, 44 catheter-days per patient [range, 1 to 395 catheter-daysper patient]), during which 69 bloodstream infections occurred(0.99 infections per 1000 catheter-days).

Eighteen variables were found to be statistically significantin univariable analyses (Table 1) and were considered for inclusionin the multivariate model. Of these, 5 were found to be independentlysignificant and were retained in the final model (Table 3).When all 69 bloodstream infections were considered, bone marrowtransplantation was associated with a significant increase ininfection events (hazard ratio, 5.8 [95% CI, 3.0 to 11.3]);this estimate was slightly higher when only first infectionswere included (hazard ratio, 6.6 [CI, 3.3 to 13.3]). The riskassociated with receipt of total parenteral nutrition (hazardratio, 4.1 [CI, 2.3 to 7.2]) was similar regardless of whetherlipids were included. Other independent risk factors were receiptof infusion therapy outside the home (hazard ratio, 3.6 [CI,2.2 to 5.9]), such as in an outpatient clinic or physician'soffice; therapy through a multilumen ( $≥$ 2 lumens) catheter (hazardratio, 2.8 [CI, 1.7 to 4.7]); and previous bloodstream infection,either before or during the study (hazard ratio, 2.5 [CI, 1.5to 4.2]). Interaction terms between time and each of these variableswere nonsignificant, indicating that the proportional hazardsassumption was appropriate. These five variables also remainedstatistically significant in models that excluded bloodstreaminfection caused by low-virulence organisms (analysis basedon 48 events) and in models that included only bloodstream infectiondiagnosed from a peripheral blood culture (analysis based on34 events) (data not shown).

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Table 3. Final Model of Independently Significant Risk Factors for Bloodstream Infections during Home Infusion Therapy

Bloodstream infection rates per 1000 catheter-days were 0.16(4 infections during 25 019 catheter-days) for patients withnone of these five risk factors, 0.46 (13 infections during28 039 catheter-days) for those with one risk factor, 2.22 (29infections during 13 075 catheter-days) for those with two riskfactors, and 6.77 (23 infections during 3399 catheter-days)for patients with three or more risk factors.

Because receipt of infusion therapy outside the home was a strongrisk factor for bloodstream infection, we explored diagnosesin 264 patients receiving such therapy. Of these patients, 132(50%) had infections other than HIV, 117 (44%) had cancer, 19(7%) had HIV infection, and 14 (5%) had undergone bone marrowtransplantation. The total is more than 100% because some patientshad more than one diagnosis.

Bloodstream infection rates and adjusted hazard ratios for selectedfactors that were not independently significant are shown inTable 4. The rate of bloodstream infection was similar at theCleveland and Toronto sites. Compared with implanted ports,centrally inserted venous catheters carried a higher but nonsignificantrisk (hazard ratio, 2.4 [CI, 0.8 to 7.4]). Time since catheterinsertion did not influence the risk for bloodstream infection;compared with the reference category (hazard ratio, 1.0) of1 to 33 days, catheters in place for 244 days or longer carrieda hazard ratio of 0.6 [CI, 0.3 to 1.5]. The hazard ratio waslower during periods of antibacterial treatment (hazard ratio,0.4 [CI, 0.1 to 1.1]) and when chlorhexidine was used at dressingchanges (hazard ratio, 0.6 [CI, 0.2 to 1.3]) and was higherwhen transparent dressings were used (hazard ratio, 1.3 [0.8to 2.1]), but these effects were not statistically significant.

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Table 4. Selected Factors That Were Not Independently Associated with Bloodstream Infections during Home Infusion Therapy

Needleless devices were used during 76% of total catheter-days;however, these devices did not increase risk (hazard ratio,0.9 [CI, 0.5 to 1.6]) (Table 4). The most common interval forchanging of needleless devices was four times per month; riskwas elevated when the devices were changed less frequently (hazardratio, 2.2 [CI, 0.9 to 5.7]), but this was not statisticallysignificant.

Discussion

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Methods
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Discussion
Author & Article Info
References

In a prospective study of 827 patients receiving home infusiontherapy through central or midline catheters, we found fiveprobable risk factors for bloodstream infection. Patient-associatedrisk factors were recent bone marrow transplantation and previousbloodstream infection. Patient care-related features were receiptof total parenteral nutrition, administration of intravenoustherapy in an outpatient setting other than the home (such asa hospital clinic or physician's office), and use of a multilumencatheter. The rate of bloodstream infection increased as thenumber of risk factors present increased, ranging from 0.16infections per 1000 catheter-days in patients with no risk factorsto 6.77 infections per 1000 catheter-days in patients with threeor more risk factors.

Bone marrow transplantation increases susceptibility to bacterialinfections, primarily during the neutropenic period in the first1 to 2 months after transplantation (9, 10). Our data do notexplain how bone marrow transplantation increases risk, buta previous study also identified neutropenia as a risk factorfor bloodstream infection (11). We recorded leukocyte countsof patients at the time of bloodstream infection but not inpatients without bloodstream infection; thus, we could not evaluateleukopenia or neutropenia as a risk factor for bloodstream infection.Neutrophil counts should be recorded in future studies of thistopic.

Infusion therapy outside the home, which was received by patientswith diverse diagnoses, has not been reported previously asa risk factor for bloodstream infection. It may be a markerfor increased catheter manipulation and line entries, or itmay indicate poor infection-control technique in outpatientclinics or physician's offices. Receipt of total parenteralnutrition (3, 12), receipt of therapy through a multilumen catheter(13), and previous bloodstream infection (4) have been associatedpreviously with bloodstream infection. In our study, HIV infectionmay have provided an apparently protective but nonsignificanteffect; however, patients with HIV may have received oral antibioticprophylaxis against opportunistic infections, may have beenbetter educated, and may have had greater experience with infusiontechniques.

Our findings may differ from those of previous studies becauseof variation in study samples, definitions of bloodstream infectionand other study methods, infection-control practices, and typesof catheters and other devices used. In contrast to some recentinvestigations (3-7), we found no association between needlelessdevices and bloodstream infection. Although the number of patientsin our study in whom needle access devices were used was small,the hazard ratio CI of 0.5 to 1.6 for this variable is consistentwith at most a modest risk.

We found no significant difference in risk among types of catheterused, but centrally inserted venous catheters had the highesthazard ratio (2.4 [CI, 0.8 to 7.4]) and implanted ports hadthe lowest hazard ratio (1.0 [reference category]). The hazardratio for peripherally inserted central catheters was intermediate(1.5 [CI, 0.3 to 6.8]). Peripherally inserted central cathetersare a sensible option for ambulatory delivery of total parenteralnutrition, antibiotics, and chemotherapy because of their relativeease of insertion and removal, as well as their relatively lowrates of associated infection (12).

Our findings generally agree with a recent guideline for preventingcatheter-related bloodstream infections (14). The guidelinerecommends using single-lumen catheters if possible (we founda higher risk associated with multilumen catheters), does notrecommend antibacterial ointment under dressings (we found nosignificant effect for ointment), does not specify a frequencyof dressing changes (we found no significant effect for thisfactor), and has no recommendation for or against the use oftransparent dressings (we found no significant risk associatedwith this factor, in contrast to some studies suggesting thattransparent dressings increase risk [15]).

We found that days since catheter insertion did not influencerisk for bloodstream infection; "old" catheters have a riskper day similar to that of "young" catheters. This is in agreementwith results of another recent study (16) and supports the recommendationagainst routine catheter changes (14).

Previous studies have reported a range of bloodstream infectionrates. Among patients with centrally inserted venous catheters,rates were 4.5 to 14.6 infections per 1000 catheter-days amonghospital inpatients (17) and 0.49 to 3.9 infections per 1000catheter-days among outpatients (11, 18, 19). Among patientswith peripherally inserted central catheters, rates were 0 to1.6 infections per 1000 days (12, 20-22).

Compared with data from hospital studies (23), we report a generallysimilar distribution of species causing bloodstream infectionbut found a higher proportion of corynebacteria (6% comparedwith <1%). This finding may indicate increasing importanceof these low-virulence organisms or that some of the episodesthat we classified as bloodstream infections represented cathetercolonization or contamination of the blood culture specimen.We reported a higher proportion of polymicrobial bloodstreaminfections (20%) than that in recent studies in hospital (14%)(24) and outpatient (11%) (5) settings.

The external validity of our study—the ability to generalizeresults to other populations—may be limited because enrolledpatients were more likely than nonenrolled patients to havereceived transplants or total parenteral nutrition and thereforemay have been at higher risk for bloodstream infection. Theinternal validity was limited by the fact that this was an observationalstudy without randomization; thus, potential confounding factorsmay not have been balanced among various comparison groups.In addition, the sample size limited the power to detect smalleffects. Some bacteremias that were diagnosed from blood culturesdrawn through the catheter may have been due to catheter colonizationrather than to bloodstream infection, but 5 major risk factorsremained significant when these events were excluded. Althoughmany potential risk factors were examined, it is unlikely thatthe reported associations were spurious, as evidenced by thehigh hazard ratios and the highly significant P values. Somebloodstream infections may have been missed if catheters wereremoved, possibly because of occlusion, and blood cultures werenot performed. Finally, our study contained a small number ofinfections relative to the number of candidate risk factors.Although our final model included only 5 risk factors, we startedwith 18 candidate variables. Future studies with more data willneed to replicate our finding that these 5 factors are significantpredictors in multivariable analyses.

Strengths of our study are its large sample size and prospectivecohort design. In addition, data on several potential risk factorswere collected in a time-dependent manner, allowing a detailedmultivariable analysis that adjusted for potential confoundingvariables and accounted for time at risk.

These data help to define the frequency of and risk factorsfor bloodstream infection during home infusion therapy. Of thefive independently significant risk factors identified, two—useof multilumen catheters and receipt of infusion therapy outsidethe home—were associated with most bloodstream infectionsand may be modifiable. Interventions aimed at these two factorsmay have the greatest impact in reducing bloodstream infections.Multilumen catheters (associated with 42 of 69 bloodstream infections)are required to administer some infusion regimens, but the riskassociated with their use should be carefully weighed so thatthey are not used unnecessarily. Receipt of infusion therapyoutside the home (associated with 36 bloodstream infections)is a newly reported risk factor; further studies are neededto confirm this association and to determine the specific mechanismby which it may increase bloodstream infections. In the interim,personnel in outpatient clinics and physician offices shouldreview infection-control procedures and ensure that proper techniqueis used when catheters are accessed.

Author and Article Information

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From the Centers for Disease Control and Prevention, Atlanta, Georgia; Mount Sinai/Princess Margaret Hospitals, Toronto, Ontario, Canada; and The Cleveland Clinic Foundation, Cleveland, Ohio.

Acknowledgments: The authors thank Demie Lyons, RN, PNP, ofPharMark Corp., Arlington, Virginia, and Thomas Westrich, RPh,of Coram Healthcare, Inc., for helping to design the project;and Barbara Godfrey, RN, Mount Sinai/Princess Margaret Hospitals,Toronto, Canada, for assistance in data collection.

Requests for Reprints: Jerome I. Tokars, MD, MPH, HospitalInfections Program, Centers for Disease Control and Prevention,1600 Clifton Rd, MS E-69, Atlanta, GA 30333

Current Author Addresses: Drs. Tokars and Jarvis: HospitalInfections Program, Centers for Disease Control and Prevention,1600 Clifton Road, MS E-69, Atlanta, GA 30333.

Dr. Cookson: Centers for Disease Control and Prevention, 1600Clifton Road, E-03, Atlanta, GA 30333.

Ms. McArthur and Dr. McGeer: Department of Microbiology, Room1460, Mount Sinai Hospital, 600 University Avenue, Toronto,Ontario M5G 1X5, Canada.

Ms. Boyer: 2339 Clague Road, Westlake, OH 44145.

References

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JPEN J Parenter Enteral Nutr, November 1, 2005; 29(6): 408 - 412.
[Abstract] [Full Text] [PDF]

M. Zurcher, M. R. Tramer, and B. Walder
Colonization and Bloodstream Infection with Single- Versus Multi-Lumen Central Venous Catheters: A Quantitative Systematic Review
Anesth. Analg., July 1, 2004; 99(1): 177 - 182.
[Abstract] [Full Text] [PDF]

L. A. Gorski
Making a Commitment to Clinical Data
Home Health Care Management Practice, April 1, 2004; 16(3): 206 - 211.
[Abstract] [PDF]

J. S. Yogaraj, A. M. Elward, and V. J. Fraser
Rate, Risk Factors, and Outcomes of Nosocomial Primary Bloodstream Infection in Pediatric Intensive Care Unit Patients
Pediatrics, September 1, 2002; 110(3): 481 - 485.
[Abstract] [Full Text] [PDF]

L. J. Walshe, S. F. Malak, J. Eagan, and K. A. Sepkowitz
Complication Rates Among Cancer Patients With Peripherally Inserted Central Catheters
J. Clin. Oncol., August 1, 2002; 20(15): 3276 - 3281.
[Abstract] [Full Text] [PDF]

E. Steiger and C. Ireton-Jones
The Evolution of Home Parenteral Nutrition in the United States
Nutr Clin Pract, August 1, 2001; 16(4): 236 - 239.
[PDF]

S. J. Rehm, D. R. Graham, L. Srinath, P. Prokocimer, M.-P. Richard, and G. H. Talbot
Successful administration of quinupristin/dalfopristin in the outpatient setting
J. Antimicrob. Chemother., May 1, 2001; 47(5): 639 - 645.
[Abstract] [Full Text] [PDF]

				C. Compher, M. Pazianas, S. Benedict, J. C. Brown, B. P. Kinosian, and M. Hise Systemic Inflammatory Mediators and Bone Homeostasis in Intestinal Failure JPEN J Parenter Enteral Nutr, March 1, 2007; 31(2): 142 - 147. [Abstract] [Full Text] [PDF]

				D. G. Maki, D. M. Kluger, and C. J. Crnich The Risk of Bloodstream Infection in Adults With Different Intravascular Devices: A Systematic Review of 200 Published Prospective Studies Mayo Clin. Proc., September 1, 2006; 81(9): 1159 - 1171. [Abstract] [Full Text] [PDF]

				W. J. Chwals Vascular Access for Home Intravenous Therapy in Children JPEN J Parenter Enteral Nutr, January 1, 2006; 30(1_suppl): S65 - S69. [Abstract] [Full Text] [PDF]

				J. T. Watson, R. C. Jones, A. M. Siston, J. R. Fernandez, K. Martin, E. Beck, S. Sokalski, B. J. Jensen, M. J. Arduino, A. Srinivasan, et al. Outbreak of Catheter-Associated Klebsiella oxytoca and Enterobacter cloacae Bloodstream Infections in an Oncology Chemotherapy Center Arch Intern Med, December 12, 2005; 165(22): 2639 - 2643. [Abstract] [Full Text] [PDF]

				A. Chang, R. Enns, O. Saqui, N. Chatur, S. Whittaker, and J. P. Allard Line Sepsis in Home Parenteral Nutrition Patients: Are There Socioeconomic Risk Factors? A Canadian Study JPEN J Parenter Enteral Nutr, November 1, 2005; 29(6): 408 - 412. [Abstract] [Full Text] [PDF]

				M. Zurcher, M. R. Tramer, and B. Walder Colonization and Bloodstream Infection with Single- Versus Multi-Lumen Central Venous Catheters: A Quantitative Systematic Review Anesth. Analg., July 1, 2004; 99(1): 177 - 182. [Abstract] [Full Text] [PDF]

				L. A. Gorski Making a Commitment to Clinical Data Home Health Care Management Practice, April 1, 2004; 16(3): 206 - 211. [Abstract] [PDF]

				J. S. Yogaraj, A. M. Elward, and V. J. Fraser Rate, Risk Factors, and Outcomes of Nosocomial Primary Bloodstream Infection in Pediatric Intensive Care Unit Patients Pediatrics, September 1, 2002; 110(3): 481 - 485. [Abstract] [Full Text] [PDF]

				L. J. Walshe, S. F. Malak, J. Eagan, and K. A. Sepkowitz Complication Rates Among Cancer Patients With Peripherally Inserted Central Catheters J. Clin. Oncol., August 1, 2002; 20(15): 3276 - 3281. [Abstract] [Full Text] [PDF]

				E. Steiger and C. Ireton-Jones The Evolution of Home Parenteral Nutrition in the United States Nutr Clin Pract, August 1, 2001; 16(4): 236 - 239. [PDF]

				S. J. Rehm, D. R. Graham, L. Srinath, P. Prokocimer, M.-P. Richard, and G. H. Talbot Successful administration of quinupristin/dalfopristin in the outpatient setting J. Antimicrob. Chemother., May 1, 2001; 47(5): 639 - 645. [Abstract] [Full Text] [PDF]