Pathogenesis and Treatment of HIV-Associated Renal Diseases: Lessons from Clinical and Animal Studies, Molecular Pathologic Correlations, and Genetic Investigations

Established in 1927 by the American College of Physicians

Article

	Table of Contents

	Abstract of this article Free

	PDF of this article (PDFs free after 6 months)

	Figures/Tables List

	Articles citing this article

Services

	Send comment/rapid response letter

	Notify a friend about this article

	Alert me when this article is cited

	Add to Personal Archive

	Download to Citation Manager

	ACP Search

	Get Permissions

Google Scholar

	Search for Related Content

PubMed

Articles in PubMed by Author:

	Kimmel, P. L.

	Kopp, J. B.

NIH CONFERENCE

Pathogenesis and Treatment of HIV-Associated Renal Diseases: Lessons from Clinical and Animal Studies, Molecular Pathologic Correlations, and Genetic Investigations

Paul L. Kimmel, MDModerator:; Laura Barisoni, MDDiscussants:; and Jeffrey B. Kopp, MD

5 August 2003 | Volume 139 Issue 3 | Pages 214-226

HIV infection is associated with several renal syndromes, includingacute renal failure. Chronic renal failure directly linked toHIV infection includes thrombotic microangiopathic renal diseases,immune-mediated glomerulonephritides, and HIV-associated nephropathy.A renal biopsy may be necessary for diagnosis. The developmentof HIV-associated nephropathy has been definitively linked torenal cellular infection, but the disease affects only a minorityof patients, typically men of African descent. Therefore, factorsdetermining disease expression in infected patients must nowbe emphasized.

The pathogenic mechanisms involved in HIV-associated renal diseaseremain obscure. Genetic factors, as well as renal cellular responses,mediated by HIV proteins (including an immune-activated microenvironment)capable of presenting antigen in susceptible hosts probablyexplain most cases. HIV-associated nephropathy has a characteristicpathologic phenotype, including glomerular, tubular, and interstitialchanges, and ultrastructural findings. Infection of the glomerularepithelial cell, or podocyte, and consequent structural andbiochemical changes may be pivotal in pathogenesis. The HIV-1transgenic mouse is an important model for understanding diseasepathogenesis, particularly the role of HIV proteins in mediatingrenal tissue injury.

Rigorously controlled randomized trials have not evaluated treatment,but corticosteroids and angiotensin-converting enzyme inhibitorshave been used. Highly active antiretroviral therapy seems tohave decreased the incidence of end-stage renal disease relatedto HIV infection and, in case reports, to have improved renalfunctional and pathologic outcomes of HIV-associated nephropathy.Outcomes in patients undergoing hemodialysis and peritonealdialysis have improved, and current research focuses on renaltransplantation for treatment of HIV-infected patients.

Dr. Paul L. Kimmel (Division of Hematologic, Kidney and UrologicDiseases, National Institute of Diabetes and Digestive and KidneyDiseases, National Institutes of Health [NIH], Bethesda, Maryland,and George Washington University Medical Center, Washington,DC): Renal disease associated with AIDS was first reported in1984 and 1985 in New York, New York, and Miami, Florida (1-3).Rao and colleagues from Brooklyn, New York, identified a singlerenal disease, focal segmental glomerulosclerosis, associatedwith AIDS (1), while other reports from Miami and Manhattanemphasized a spectrum of glomerular abnormalities and variousrenal syndromes seen in patients with AIDS (2, 3).

A variety of renal syndromes can complicate the course of HIVinfection (4). Clinical strategies involve diagnosing the typeof renal disease and instituting appropriate therapy. Researchneeds involve understanding the pathogenesis of individual renaldiseases that complicate HIV infection, understanding the relationshipof these diseases to infection and its treatment, and devisingtreatments for patients with chronic kidney disease.

Clinical Aspects of Renal Syndromes in HIV-Infected Patients

Acute Renal Failure

Although common causes of acute renal failure, as in uninfectedhospitalized patients, are prerenal azotemia and acute tubularnecrosis (5, 6), recent studies highlight an increased incidenceof HIV-associated thrombotic microangiopathies and rhabdomyolysis(7-9); the latter may stem from statin use in patients withcomplications of antiretroviral therapy (10-14). Opportunisticinfections complicating the viral illness, such as tuberculosis,cytomegalovirus infection, and fungal infections, and complications,such as lymphoma and Kaposi sarcoma, are associated with structuralanatomic abnormalities, renal insufficiency, and acute renalfailure (6, 8). Chronic kidney disease, such as thrombotic thrombocytopenicpurpura, associated with HIV infection, can also mimic acuterenal failure (4, 6, 15). Drugs used to treat superinfectionsassociated with HIV infection (for example, antibiotics, antifungals,and antivirals) and antiretroviral drugs to treat HIV infection(for example, indinavir and ritonavir) (16) are associated withthe development of interstitial nephritis and nephrotoxicity.Antibiotics commonly cause acute interstitial nephritis, whileaminoglycosides, amphotericin, and foscarnet cause acute tubularnecrosis. The nucleoside phosphonate analogues adefovir andcidofovir cause proximal renal tubular injury (16). Abacavir(17) and tenofovir (18, 19) are implicated in the developmentof tubular injury and renal failure. Sulfadiazine, acyclovir,and indinavir cause crystalluria and, occasionally, intrarenalobstruction (20). Indinavir is associated with several nephrologicsyndromes, such as dysuria, acute and chronic interstitial nephritis(including tubular atrophy and interstitial fibrosis), and nephrolithiasis;nelfinavir has been linked to the development of nephrolithiasis(10, 16, 21-23). Leukocyturia is associated with progressiverenal disease in patients treated with indinavir (22, 24).

Chronic Renal Disease: End-Stage Renal Disease

Currently, HIV-infected patients make up approximately 1% to2% of the population with end-stage renal disease (25-27) (Figure 1).The incidence geographically reflects the national distributionof AIDS and HIV infection (25, 26). The prevalence of HIV infectionin the dialysis program is probably higher because of confidentialityissues and the lack of biopsies in most patients. During thelate 1980s, the number of HIV-infected patients in the dialysisprogram was low but had tripled from 1985 to 1988 (25, 27) (Figure 1).However, subsets of the population, such as young blackmen, were at particularly high risk for developing nephropathy(28, 29). The relative risk for end-stage renal disease fromAIDS or an AIDS-defining diagnosis from 1995 to 1999 is 0.39for women compared with men (Eggers PW. Personal communication).Risk between men and women does not vary by race or ethnicity,but black patients had a relative risk of 51.1 for developingend-stage renal disease from AIDS or an AIDS-defining diagnosiscompared with white patients. Although early work suggesteda rapidly increasing number of HIV-infected patients (28), thenumber and proportion of patients undergoing dialysis who hadrenal disease attributed to HIV infection have stabilized orare decreasing (25-27) (Figure 1). Between 1995 and 1999, thenumber of new patients with HIV infection in the U.S. hemodialysisprogram ranged from 1131 to 1187 and did not rise proportionatelywith the increase in HIV infection or the U.S. dialysis population(26).

View larger version (12K):
[in this window]
[in a new window]

Figure 1. Percentage of HIV-infected patients receiving hemodialysis in the U.S. hemodialysis program. Data obtained from the Centers for Disease Control and Prevention. Reproduced with permission from reference 27, Kidney Int. 2003; 63:1618-31.

Chronic Renal Failure

The prevalence of renal disease related to HIV infection isunknown, rendering epidemiologic assessments problematic (29).The designation of chronic kidney disease in HIV-infected patientsdepends on the screening techniques used (30). Data before (30, 31)and after (32) the introduction of highly active antiretroviraltherapy suggest a prevalence of abnormal proteinuria of aboutone third, using various criteria. A European autopsy studyof HIV-infected patients, most of whom had developed AIDS, showedproteinuria in 18%, nephropathy in 36%, and renal pathologyin 43% (31). Less than 10% of a cohort of HIV-infected womenhad proteinuria or renal insufficiency at baseline, but 14%developed kidney disease during a mean 21-month follow-up (33).In a large study of HIV-infected women, viral load and stageof infection were associated with proteinuria and progressivenephropathy but presence and type of antiretroviral therapywere not (32).

Three types of chronic kidney disease are directly caused byHIV infection: HIV-associated thrombotic microangiopathies,HIV immune-mediated renal diseases, and classic HIV-associatednephropathy (4, 27). Because of improved understanding of theHIV life cycle, advances in molecular biological tissue evaluation,and the development of relevant animal models, stronger pathogenicinferences can be made about HIV-associated nephropathies comparedwith other renal diseases. Elucidating the pathogenesis of HIV-associatedrenal diseases also permits better understanding of pathogenicmechanisms underlying more common renal diseases.

HIV-Associated Thrombotic Microangiopathy

The thrombotic microangiopathies, hemolytic uremic syndromeand thrombotic thrombocytopenic purpura, are thought to occurbecause of endothelial cell dysfunction partially mediated byHIV proteins (4, 15, 34-36). Renal cellular apoptosis (4, 15, 34, 37),as well as inhibition of von Willebrand factor–cleavingprotease (38), may play key pathogenic roles. The disease spectrumis characterized by a pentad of findings with variable expression:fever, neurologic dysfunction, thrombocytopenia, microangiopathichemolytic anemia, and renal insufficiency with hematuria. High-levelproteinuria is uncommon, which helps differentiate these syndromesfrom immune-mediated diseases and HIV-associated nephropathy(4). However, nephrotic-range proteinuria does occur (39-41),perhaps because of the coexistence of two diseases (41). Althoughspontaneous remissions occur (40), the renal disease often resiststreatment. Treatment with glucocorticoids (41, 42), plasma andimmunoglobulin infusions, plasmapheresis, antiplatelet drugs,vincristine, and splenectomy has variable success (15, 27),but lack of controlled trials precludes evidence-based recommendations.

HIV-Associated Immune-Mediated Glomerulonephritides

Autopsy and biopsy series in HIV-infected patients with renaldisease have established a prevalence of proliferative glomerulonephritisof 10% to 80% (42-49). Immune complex glomerulonephritis associatedwith HIV infection has several different histologic presentations(43, 49), including proliferative, lupus-like, and mixed proliferativeor sclerotic forms (43). Other types of glomerulonephritis,such as membranoproliferative glomerulonephritis, membranousnephropathy, fibrillary and immunotactoid glomerulonephritis,and postinfectious glomerulonephritis, also occur in HIV-infectedpatients (43, 45, 46, 49-52). The renal disease, however, maynot be intimately associated with HIV infection. Rather, itmay be a consequence of coexistent infection, such as renaldisease related to hepatitis C or B (49, 53-55), a responseto infection in patients with disordered humoral immunity (49, 56),or a coincidental finding (49). A renal biopsy with immunochemicaland molecular biological analyses is necessary to make a preciseetiologic diagnosis, but this is usually not possible in clinicalpractice. By using classic research techniques, we showed thatthe immune response to HIV infection could culminate in specificHIV immune-mediated glomerulonephritis (57).

IgA nephropathy occurs in HIV-infected patients (4, 49, 58, 59).Its incidence and prevalence are unknown. In an autopsystudy, 7.75% of persons with AIDS had diffuse mesangial IgAdeposits (60). IgA nephropathy in HIV infection seems to berelatively common in men of European descent but uncommon inpeople of African descent (27, 49, 60), as in uninfected populations(61). We showed that IgA nephropathy in two patients was theresult of an autoimmune reaction to HIV peptides (59). HIV-associatedIgA nephropathy is generally indolent, characterized by proteinuria,hematuria, and mild renal insufficiency.

European and Asian case series of patients with HIV infectionand renal disease who underwent biopsies or autopsies show thatpatients of European descent typically have glomerulonephritis,while patients of African descent in the same centers usuallyhave HIV-associated nephropathy (31, 43, 45-49). These disparitiesand the clustering of renal disease in families of patientswith HIV infection and end-stage renal disease (62) suggesta genetic component for developing both HIV-associated immune-mediatedrenal diseases and HIV-associated nephropathy.

Remarkable responses have been reported in patients with immune-mediatedrenal diseases treated with angiotensin-converting enzyme (ACE)inhibitors, glucocorticoids, or antiretroviral therapy (51, 63-65),but properly designed randomized, controlled trialshave not assessed such therapies.

Classic HIV-Associated Nephropathy

Although some researchers suggest that HIV-associated nephropathycomprises a spectrum of mesangial diseases and matrix productiondisorders (66), variants of focal segmental glomerulosclerosis,including collapsing glomerulopathy, were reported in most HIV-infectedpatients with renal disease who underwent renal biopsy (4, 27, 67, 68).HIV-associated nephropathy is characterized by large,echogenic kidneys on ultrasonography, nephrotic-range proteinuria,and renal insufficiency. Although it has been argued that HIV-associatednephropathy is a late complication (67, 69), it can clearlyoccur at any stage of HIV infection and is occasionally thepresenting manifestation of infection (70-72). The pathologicfindings are pathognomonic (66-68, 73, 74). Although clinicalfindings are suggestive, a biopsy is necessary for diagnosis.Before the introduction of highly active antiretroviral therapyin 1996, HIV-associated nephropathy was typified by an extremelyrapid progression that was thought to be inexorable.

Pathogenic Considerations

The pathogenesis of HIV-associated nephropathy is unknown, butthree lines of evidence definitively link the disease to viralinfection: 1) the finding of HIV-associated nephropathy in infectedinfants of HIV-infected mothers [75]; 2) the reproduction ofthe disease in HIV-1 transgenic mice, rats, and simian modelsof retroviral infection [15, 76-79]; and 3) reports of reversalof renal histologic and laboratory abnormalities in a smallset of patients with biopsy-proven HIV-associated nephropathyafter highly active antiretroviral therapy (70, 72).

We showed the ubiquitous presence of HIV DNA in renal tissueof HIV-infected patients (44), but only recently has human renalviral infection been demonstrated by the localization of HIV-1messenger RNA in renal tissue, specifically glomerular and tubularepithelial cells (72, 80-82). However, proteinuria is presentin less than half of HIV-infected patients (30-33), and advancedstages of chronic kidney disease are an uncommon complicationof HIV infection (4, 27, 66, 67). Therefore, factors other thansimple infection of renal cells or the infiltration of infectedimmune cells in renal tissue probably mediate the expressionof nephropathy (4, 44). Large-scale clinical epidemiologic andpathologic studies of the relationship of renal HIV infectionto the expression of disease, with the proper positive and negativecontrols, remain to be performed.

Cytokines and growth factors, produced by infiltrating immuneor renal cells, undoubtedly play roles in mediating diseasepathogenesis in susceptible hosts through effects on renal cellsor the viral life cycle. The presence of an immune cell infiltratein the renal tissue of patients with HIV-associated nephropathyremains unexplained, but clinicopathologic data implicate themacrophage in the pathogenesis of HIV-associated nephropathy(83). Chemokines mediate infiltration of tissue by monocytes,macrophages, lymphocytes, neutrophils, and eosinophils and havebeen implicated in nephropathogenesis (84). Certain chemokinereceptors function as second receptors for the engagement ofHIV virions and the cell membrane (85). Mutations in chemokinereceptor proteins are associated with resistance to HIV infectionand improved prognosis (86). Chemokine receptor RNA has beendetected in renal tissue (84, 87, 88), but detecting chemokinereceptors in HIV-associated nephropathy tissue is limited toinfiltrating immune cells (89). We investigated the relationshipof tissue transforming growth factor-ß (90) and chemokines(91) to the presence of nephropathy by comparing biopsy specimensfrom patients with HIV-associated nephropathy, HIV-associatedglomerulonephritis, and idiopathic focal glomerulosclerosiswithout HIV infection, with appropriate controls. Chemokinelevels were increased in renal tissue from patients with HIVinfection regardless of the presence of renal disease (91).This finding suggests that chemokines might help prevent productiveinfection of renal cells by interacting with renal chemokinereceptors, thereby decreasing the number of renal cells infectedand the subsequent expression of nephropathy. Tissue proteinsassociated with antigen presentation and response to infection,including MHC class II proteins, interferon- ${alpha}$ , and interferon- ${gamma}$ receptor protein, were specifically associated with HIV-associatednephropathy, suggesting that genetic susceptibility, the hostresponse, and a microenvironment characterized by immune activationare critical to nephropathogenesis (Figure 2). The finding ofhigh levels of interferon- ${alpha}$ is consistent with the pathologicfeature of tubuloreticular inclusions (4, 68, 73, 74, 91). Human(92) and animal (93) studies suggest that apoptosis, perhapsmediated by HIV proteins, plays an important role in nephropathogenesis.A complex interrelationship probably exists among renal infection,effects on renal cell matrix biology, cytokine, growth factor,and chemokine responses, mediated by host factors (includinggenetic susceptibility and socioeconomic status) leading tothe development of HIV-associated nephropathy.

View larger version (23K):
[in this window]
[in a new window]

Figure 2. Interferon- ${alpha}$ protein expression in renal tissue compartments. Interferon- ${alpha}$ protein was assessed in microdissected renal glomerular and interstitial tissue from 6 patients with HIV-associated nephropathy, 4 patients with HIV-associated immune-mediated glomerulonephritis, 3 HIV-infected patients who died without autopsy evidence of renal disease, 9 patients with idiopathic focal segmental glomerulosclerosis in the absence of HIV infection, and renal tissue of uninfected patients without clinical or pathologic evidence of renal disease by high-performance immunoaffinity chromatography and chemiluminescent enzyme-linked immunosorbent assay. Renal interstitial and glomerular interferon- ${alpha}$ protein levels were significantly higher in renal tissue from patients with HIV-associated nephropathy than in tissue from all other groups (P = 0.002; analysis of variance). A similar pattern was noted for nonpolymorphic major histocompatibility II locus and interferon- ${gamma}$ receptor protein levels. Error bars indicate SEs. *P = 0.002.

Treatment of HIV-Associated Nephropathy

No rigorously controlled randomized trials have evaluated treatmentof HIV-associated nephropathy (27, 94). Glucocorticoid therapyproduced impressive decreases in urinary protein excretion andimproved renal function (95), but treatment before the introductionof highly active antiretroviral therapy was associated witha high prevalence of serious complications (94-97). More recentstudies suggest that steroid treatment is associated with improvedrenal functional outcomes and less morbidity, perhaps secondaryto concomitant highly active antiretroviral therapy (96-98).Two studies completed before the introduction of highly activeantiretroviral therapies suggest that ACE inhibitors have clinicallysignificant effects on renal survival (99, 100). This effectwas confirmed in the HIV-1 transgenic mouse (101). The mechanismof action of these drugs is unknown. Steroids may decrease theassociated component of interstitial inflammation (41, 94),while ACE inhibitors may affect interstitial immune cellularfunction and the generation of tissue cytokines (4, 94, 99).

Antiretroviral drug therapy has been associated with beneficialeffects on renal functional status, morbidity, and mortality(4, 27, 94, 102-104). In patients treated with captopril, useof antiretrovirals was independently associated with improvedrenal survival (99). Two dramatic case reports suggest thattreating patients with HIV-associated nephropathy with highlyactive antiretroviral therapy may result in remission of bothrenal pathologic and functional abnormalities (70, 72), althoughthe kidney may remain a reservoir of infection (72, 81, 82).Outcomes of HIV-infected patients treated with hemodialysisand peritoneal dialysis have improved and the incidence of HIVinfection in the dialysis program seems to have decreased concomitantlywith the introduction in 1996 of highly active antiretroviraltherapy (25-27, 105, 106) (Figure 1). Although the immunosuppressionof HIV-infected patients is a concern, the prospect of transplantationfor carefully selected HIV-infected patients is exciting butcontroversial (27, 107-111). Some of the immunosuppressive medicationsused in clinical transplantation may have antiretroviral effects(27, 109). Successful transplantation in HIV-infected patientswho have received highly active antiretroviral therapy and haveundetectable viral loads has been reported in abstract form,and a multicenter study is in progress (27, 108). Murphy andcolleagues transplanted kidneys in 23 patients who were receivingantiretroviral therapy, had CD4 cell counts greater than 0.200x 10⁹ cells/L, and had undetectable viral loads; the graft survivalrate was 87% (27, 108).

Approach to the HIV-Infected Patient with Chronic Kidney Disease

We believe that HIV-infected patients with chronic kidney diseaseshould be assessed by using standard clinical tools. The absenceof nephrotic-range proteinuria suggests a diagnosis other thanHIV-associated nephropathy or glomeulonephritis. The peripheralsmear should be examined in patients with acute or chronic renaldisease who have thrombocytopenia or hemolysis. A renal biopsyis necessary to diagnose HIV-associated nephropathy. This maybe a clinically significant decision for patients in whom highlyactive retroviral therapy would otherwise be deferred (112)since antiretroviral therapy can improve outcomes, but renaldiseases unrelated to HIV infection would not be expected torespond (4, 27, 44, 113). Although this recommendation is notsubstantiated by evidence from clinical trials, patients withchronic kidney disease associated with HIV infection shouldbe treated with highly active antiretroviral therapy unlessit is contraindicated. A good rationale exists for ACE inhibitorsfor patients who do not have a dramatic response to such therapy,although the effects of such combinations have not been evaluatedprospectively. In selected patients whose viral infection iscontrolled, the addition of glucocorticoids may improve renalfunction. Further study is necessary to evaluate the resultsof combinations of antiretroviral therapy, drugs that interruptthe renin–angiotensin axis, and steroids in patients withHIV-associated renal diseases. Renal transplantation is an optionfor selected patients in controlled trials.

Pathologic Features of HIV-Associated Nephropathy

Dr. Laura Barisoni (Kidney Disease Section, National Instituteof Diabetes and Digestive and Kidney Diseases, NIH, and TheJohns Hopkins University, Baltimore, Maryland): The appropriateclassification of focal segmental glomerulosclerosis is controversialand evolving. Collapsing glomerulopathy represents a subtypeof focal segmental glomerulosclerosis, distinguished by oneor more glomeruli manifesting segmental or global collapse andpodocyte hypertrophy or hyperplasia (114-117). A common associatedfeature is severe tubular injury and interstitial inflammatoryinfiltration out of proportion to the glomerular disease. Collapsingglomerulopathy may be associated with HIV-1 infection, in whichcase it is termed HIV-associated nephropathy, or it may occurwithout known viral infection. Although idiopathic collapsingglomerulopathy and HIV-associated nephropathy are similar, HIV-associatednephropathy can be distinguished by the presence of tubularmicrocysts and glomerular endothelial tubuloreticular inclusions(however, these are not always present). Both forms of collapsingglomerulopathy are believed to share common pathogenic mechanismsrelated to dysregulation of podocyte phenotype (118, 119).

Like collapsing glomerulopathy, HIV-associated nephropathy ischaracterized by wrinkling and folding of the glomerular basementmembranes (Figure 3, part A). The segmental or global collapseof the glomerular basement membrane is associated with increasesin the Bowman space. Often this space is partially or globallyoccupied by large podocytes, with pale cytoplasm containingprotein-reabsorption droplets. These cells are arranged in layersaround the collapsed areas, forming pseudocrescents. Glomerulardamage is associated with tubular atrophy and flattening andregeneration of the tubular epithelium (Figure 3, part B). Interstitialinflammation and fibrosis are generally severe.

View larger version (101K):
[in this window]
[in a new window]

Figure 3. Histopathologic characteristics of HIV-associated nephropathy in humans and transgenic mice. Human HIV-associated nephropathy: A. A glomerulus shows global collapse of capillary lumina. The glomerular basement membranes are wrinkled and folded, and the urinary space is occupied by proliferating podocytes forming pseudocrescents. Numerous protein reabsorption droplets are present in the podocyte cytoplasm, and this cytoplasm is more abundant than normal (silver staining; original magnification, x60). B. Tubulointerstitial damage includes interstitial fibrosis with inflammation, tubular atrophy, and microcysts. Eosinophilic casts are present in the dilated tubular lumina (silver staining; original magnification, x40). C. Ultrastructural analysis shows a collapsed glomerular capillary. Note the wrinkling of the glomerular basement membrane. Podocytes (P) have lost foot processes and primary processes, and their cell body sits directly on the glomerular basement membrane. There is focal detachment of podocytes from the underlying glomerular basement membrane and new matrix deposition (asterisks). (Original magnification, x8000.) Membrane nephropathy in HIV-1 transgenic mice: D and E. Immunostaining for synaptopodin in wild-type (D) and HIV-1 transgenic mice (E): All the glomeruli are stained for synaptopodin in kidneys from wild type (D). No staining is noted in the kidney of the HIV-1 transgenic mice (E). (Original magnification, x20.) F and G. Immunostaining for adducin (F) and Na⁺, K⁺–adenosine triphosphatase (G) in HIV-1 transgenic mice: No basolateral staining is noted in this dilated tubule, whereas the nondilated tubules display a delicate basolateral staining (brown). (Original magnification, x40.).

In many glomerular diseases, proteinuria is associated withpodocyte foot process effacement and reorganization and withcondensation of the actin cytoskeleton; the latter manifestsas dense intracytoplasmic structures lying adjacent to the glomerularbasement membrane. HIV-associated nephropathy podocyte structureis different (Figure 3, part C). Podocytes lose their foot andprimary cytoplasmic processes, so the cell body rests directlyon the glomerular basement membrane. The actin cytoskeletonis essentially absent. These features resemble those of immaturepodocytes in the developing glomerulus, supporting the hypothesisthat cellular dedifferentiation has occurred. In some cases,podocytes detach and new extracellular matrix deposits fillthe resulting space (118).

Epithelial Cell Phenotype in HIV-Associated Nephropathy

In all forms of focal glomerulosclerosis and in HIV-associatednephropathy, expression of maturity markers, such as synaptopodin,glomerular epithelial protein 1, podocalyxin, C3b receptor,and common acute lymphoblastic leukemia antigen, is lost inthe areas of sclerosis or collapse (Figure 3, parts D and E)(118). In other forms of focal glomerulosclerosis, this phenomenonmay result from parietal epithelial cell migration from theBowman capsule. In HIV-associated nephropathy, this phenomenonmay reflect dedifferentiation of podocytes overlying areas ofcollapse. The loss of actin-based cytoskeleton observed on ultrastructuralanalysis is reflected by the absence of synaptopodin staining,which also occurs in podocytes overlying noncollapsed glomeruli;this finding suggests that cellular phenotypic alteration precedesglomerular injury. Moreover, podocalyxin, normally expressedin both podocytes and endothelial cells, is lost exclusivelyin podocytes, suggesting that HIV-associated nephropathy isa selective podocyte disease.

In HIV-associated nephropathy, the podocyte phenotype is notonly dedifferentiated but also dysregulated, reflected by lossof expression of Wilm tumor protein 1, a podocyte marker presentat all stages of glomerular development (118). In idiopathiccollapsing glomerulopathy, dysregulated podocytes may expressproteins that are more typically expressed by other cells, suchas macrophages, in a process called transdifferentiation (120).Unlike all other diseases characterized by podocyte injury,dysregulated podocytes in patients with HIV-associated nephropathyor idiopathic collapsing glomerulopathy proliferate and alsoundergo apoptosis (120, 121). The reentry into the cell cyclecoincides with the loss of expression of cyclin D1 and cyclin-dependentkinase inhibitors, p27 and p57, together with reexpression ofcyclin A and Ki-67 and the de novo expression of p21 (122).

Podocytes have several functions (123). The podocyte slit diaphragmcontributes to the glomerular filtration barrier, limiting urinaryalbumin and large-molecular-weight protein excretion. Podocytesparticipate in laying down and remodeling the glomerular basementmembrane. Podocytes may have structural functions within theglomerulus, maintaining capillary loop structure against boththe ballooning force of hydrostatic pressure and the contractileforce of mesangial cells. It is not surprising that dedifferentiatedpodocytes may fail to perform one or more of these functions.Loss of the slit diaphragms (foot process effacement) is associatedwith proteinuria. The dedifferentiated podocyte may contributeto glomerular collapse by shifting synthesis from collagen IV ${alpha}$ 3, ${alpha}$ 4, and ${alpha}$ 5 chains, typical of the adult glomerular basementmembrane, to those typical of its fetal composition (collagenIV ${alpha}$ 1 and ${alpha}$ 2 chains), which are present in the glomerular basementmembrane in HIV-associated nephropathy. Finally, the pressureof the expanding podocyte cell mass that makes up a pseudocrescentmay contribute to capillary loop collapse (Figure 4).

View larger version (35K):
[in this window]
[in a new window]

Figure 4. Model for glomerular and tubular cell injury induced by HIV-1.

Epithelial Cells Are a Target of HIV Infection

The HIV-1 transgenic mouse model of HIV nephropathy, developedat the NIH, directly linked the expression of HIV-1 proteinsto altered cellular phenotype (124). HIV-1 transgenic mice developa renal disease similar to HIV-associated nephropathy, includingfocal segmental glomerulosclerosis with glomerular collapse,severe tubulointerstitial damage, and tubular microcysts (76).Tubular epithelial cells lose the expression of proteins, suchas Na⁺, K⁺–adenosine triphosphatase, and adducin (119)(Figure 3, parts F and G). Two pieces of evidence link HIV geneexpression and renal parenchymal changes. In cross-transplantexperiments between wild-type and HIV-1 transgenic mice, nephropathydeveloped only in kidneys transplanted from transgenic intowild-type mice (93). Second, transgene expression was detectedin both podocytes and tubular epithelial cells before structuralalterations occurred. In renal epithelium, the detection ofthe transgene is followed by high apoptotic and proliferativeindices together with dysregulation of the phenotype, indicatinga temporal correlation between HIV-1 expression and nephropathy(121).

HIV-1 gene expression in podocytes and tubular epithelium ofmultiple nephron segments has been demonstrated in human biopsyspecimens (72, 81), suggesting a role of HIV-1 infection ininitiating pathogenesis, although the mechanism underlying cellulardamage is unknown. To support this hypothesis, recent studiesin podocytes derived from HIV-1 transgenic mice indicate a directeffect of HIV-1 gene products on the cell cycle, leading tocellular proliferation (125).

Mechanisms of HIV-Associated Renal Injury

Dr. Jeffrey B. Kopp (Kidney Disease Section, National Instituteof Diabetes and Digestive and Kidney Diseases, NIH): The mechanismsby which lentiviruses induce characteristic glomerular and tubularinjury are not well understood, but several important cluesto pathogenesis have emerged over the past decade.

Opportunistic renal infections might trigger focal segmentalglomerulosclerosis. Although it was suggested that Mycoplasmafermentans might contribute, few recent data support that hypothesis(126). We showed that the monkey polyomavirus simian virus 40is recovered more frequently from urinary cells of patientswith focal glomerulosclerosis, including idiopathic, collapsing,and HIV-associated variants, compared with patients with otherkidney diseases or healthy volunteers (127). These data areinsufficient, however, to establish a causative link betweensimian virus 40 infection and HIV-associated nephropathy.

HIV-1 probably infects lymphocytes and macrophages that enterthe kidney, which might release inflammatory lymphokines orcytokines and cause renal injury. Biopsy specimens from patientswith HIV-associated nephropathy have a striking increase inrenal transforming growth factor-ß–producingcells compared with specimens from patients with other formsof focal segmental glomerulosclerosis or other inflammatoryglomerular diseases (90, 128). Neither study conclusively identifiedthe cells responsible for producing transforming growth factor-ß.

Increasing evidence suggests that HIV-1 may infect renal parenchymalcells, producing cytopathic effects such as proliferation orapoptosis. In vitro experiments demonstrated low-level productiveinfection of cultured tubular epithelial cells (87, 129). Someinvestigators have reported infection of cultured mesangialcells (130), while others have not (131). The role of the chemokinereceptor GPR1 may be critical (132). In vitro infection of humanpodocytes, however, has not yet been described. Localizationof HIV-1 protein and RNA to renal parenchymal cells has beencontroversial. Both HIV-1 protein and nucleic acid were foundin podocytes and tubular epithelium (44, 133). Recently, Klotmanand colleagues (72, 81, 82) developed sensitive in situ hybridizationtechniques and localized viral RNA and newly retrotranscribedproviral DNA to podocytes and tubular epithelial cells (72, 81).Future work may delineate how HIV-1 infection leads tocellular abnormalities such as proliferation (podocytes) oratrophy and death (tubular epithelial cells).

HIV-1 proteins may directly injure renal parenchymal cells.In humans infected with HIV-1, overt immunodeficiency is notrequired for development of focal glomerulosclerosis, suggestingthat some lentiviral gene product might be responsible for nephropathogenesis.Experiments using HIV-1 transgenic mice show that particularHIV-1 accessory proteins can induce focal segmental glomerulosclerosisand interstitial nephritis (124, 134-136) (Table). These featuresinclude focal and segmental collapse and solidification of theglomerular capillary tuft, podocyte hyperplasia (but not glomerularendothelial tubuloreticular inclusions), microcystic tubulardilatation, tubular atrophy, mononuclear interstitial cell infiltration,proteinuria, and progressive renal dysfunction. These transgenicmice do not produce virions (since the gag and pol genes arelacking from the transgenes), demonstrating that replicatingvirus is not required for the induction of murine nephropathy.Two lines of evidence suggest that local renal HIV-1 proteinproduction is critical: Transgenic lines that do not expressthe transgene in the kidney but express it in other tissuesdo not develop renal disease (124), and nephropathy followsthe transgenic kidney in renal transplant experiments involvingtransgenic and wild-type mice (93).

View this table:
[in this window]
[in a new window]

Table. HIV-1 Transgenic Mice with Renal Disease

A provisional summary of these data suggests that the viralregulatory or accessory proteins Tat plus viral protein R (Vpr),or Vpr acting alone, may induce focal glomerulosclerosis, andNef (negative factor for viral replication) may contribute tointerstitial nephritis. These viral proteins have complex effectson host cell function. Dissecting the mechanisms of renal injuryinduced by these proteins is an area for future research. Tatis a transactivating protein that increases viral RNA production.Vpr has many effects on host cells, including G2 cell cyclearrest, regulation of apoptosis, and cytokine production, andacts as a transcriptional coactivator or corepressor, dependingon the genetic context. Nef downregulates CD4 expression. Insummary, in mice, particular viral regulatory or accessory proteinsinduce many characteristic functional and histologic changesof HIV-associated nephropathy.

Viral genetic variation might contribute to the epidemiologyof HIV-associated nephropathy, explaining why only some patientsdevelop renal disease. Partly because of the relatively higherror rate of HIV-1 reverse transcriptase, the HIV-1 genomeis highly plastic and many viral quasi-species exist. The env(envelope) gene encodes the transmembrane glycoprotein (gp)41 and the associated gp120. gp120 first binds CD4, inducinga conformational change in gp120 that facilitates its bindingto one of several co-receptor molecules, which function as chemokinereceptors in the host. CD4 independent cell infection has alsobeen described. The receptors responsible for viral entry intorenal parenchymal cells have not been well characterized. CD4has not been convincingly demonstrated on any renal parenchymalcell in vivo, although RNA has been reported in cultured tubularepithelial cells. Mesangial cell infection may be dependenton GPR1 (132). Particular viral variants may have mutationsin gp120 that facilitate entry into renal cells or have mutationsin regulatory or accessory proteins, such as Vpr or Nef, withparticular toxicity for renal cells, but few data address thisissue.

Host Genetic Variation and the Development of HIV-Associated Nephropathy

People of African descent with HIV-1 infection are at a markedlyincreased risk for focal segmental glomerulosclerosis, withan at least 18-fold increased risk compared with people of Europeandescent (137). Since a similar predilection is seen in the UnitedStates, Europe, and South America, cultural factors seem anunlikely explanation. Instead, one or more host genetic lociprobably contribute to risk, with particular risk alleles morecommon in populations of African descent. Theoretically, thesealleles might contribute to HIV-1 entry into renal parenchymalcells, potentiate toxicity of viral accessory proteins in renalcells, or heighten a fibrotic response to viral-initiated renalinjury.

A genetic mutation that contributes to HIV-associated nephropathymight be unique for this syndrome or extend to idiopathic focalsegmental glomerulosclerosis or other forms of glomerular injury.While there is no evidence that the first possibility is correct,the relative rarity of HIV-1 infection (<0.2% of the U.S.population is infected) makes it difficult to estimate the riskfor HIV-associated nephropathy among different kindreds. However,probands with HIV infection and renal disease have an increasednumber of first- and second-degree relatives with renal disease(not limited to focal glomerulosclerosis) compared with ethnicallymatched patients with HIV-1 infection without kidney disease(62). These data tend to support the second or third possibilityoutlined. At present, it seems that HIV-associated nephropathyprobably has both genetic and environmental components.

We have initiated ongoing studies comparing genetic polymorphismsamong African Americans with HIV-associated nephropathy, idiopathicfocal segmental glomerulosclerosis, and HIV-1 infection forat least 8 years but without renal disease (a hypernormal controlgroup, in that these individuals have been challenged with avirus known to induce focal glomerulosclerosis but have notdeveloped this syndrome), African-American blood donors, andEuropean-American patients with idiopathic focal segmental glomerulosclerosisand blood donors. We have performed genotyping in these individualsfor polymorphisms in various candidate genes, including thosefor chemokine receptors, chemokines, and members of the renin–angiotensin-transforminggrowth factor-ß system. To date, preliminary studiesdemonstrate that the only gene that differs between African-Americanpatients with HIV-associated nephropathy and African-Americancontrols is the gene encoding ACE (138). Patients homozygousfor an Alu insertion in intron 16 of ACE are at an increasedrisk for focal segmental glomerulosclerosis; this is true forboth African Americans with HIV-associated focal segmental glomerulosclerosisand those with idiopathic focal segmental glomerulosclerosis.In European Americans, the ACE polymorphism was not significantlyassociated with focal segmental glomerulosclerosis.

Angiotensin-converting enzyme polymorphisms have been associatedwith the incidence or rate of progression of various glomerulardiseases, including diabetes (139), IgA nephropathy (140), andidiopathic focal segmental glomerulosclerosis (141, 142) inAsian patients, but all these studies suggest that patientshomozygous for the intron 16 deletion allele are more susceptible.Of interest, these studies have included few African Americans.Unlike other populations, in African Americans, there is nocorrelation between intron 16 polymorphism and serum ACE level(143). We interpret these data to suggest that, in African Americans,the intron 16 polymorphism is in linkage disequilibrium withone or more mutations that contribute to focal segmental glomerulosclerosisrisk.

Conclusions

Much has been learned about the pathogenesis and treatment ofHIV-associated renal diseases because of the development ofanimal models and the molecular evaluation of clinical samples.Although the pathogenesis of HIV-associated nephropathy is clearlylinked to the viral illness, over the next decade we must determinehow infection results in the development of disease. HIV peptidesrather than infection may be more important in nephropathogenesis.We must determine why some patients are susceptible to diseasedevelopment and others are not. Genetic factors, the host response,and effects of HIV peptides on podocytes, on renal cellularapoptosis, and on the ability to present antigen may be criticalto pathogenesis. Although highly active antiretroviral therapywill play an important role in preventing and treating HIV-associatednephropathy, well-designed and -controlled clinical trials arenecessary to determine the roles of therapy with glucocorticoidsand ACE inhibitors. Knowledge about the treatment of HIV-infectedpatients with renal transplantation and proper treatment ofother HIV-associated renal diseases is rudimentary.

Author and Article Information

Top
Author & Article Info
References

From George Washington University Medical Center, Washington, DC, and National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, Maryland.

Grant Support: Dr. Kimmel was supported by grant RO1-DK-40811from the National Institute of Diabetes and Digestive and KidneyDiseases.

Potential Financial Conflicts of Interest: None disclosed.

Requests for Single Reprints: Paul L. Kimmel, MD, Divisionof Renal Diseases and Hypertension, Department of Medicine,George Washington University Medical Center, 2150 PennsylvaniaAvenue NW, Washington, DC 20037.

An edited summary of a Clinical Staff Conference Grand Roundsheld on 27 June 2001 at the National Institutes of Health, Bethesda,Maryland.

Authors who wish to cite a section of the conference and specificallyindicate its author may use this example for the form of thereference:

Barisoni L. Pathologic features of HIV-associated nephropathy.In: Kimmel PL, moderator. Pathogenesis and treatment of HIV-associatedrenal diseases: lessons from clinical and animal studies, molecularpathologic correlations, and genetic investigations.

Current Author Addresses: Dr. Kimmel: Division of Renal Diseasesand Hypertension, Department of Medicine, George WashingtonUniversity Medical Center, 2150 Pennsylvania Avenue NW, Washington,DC 20037.

Drs. Barisoni and Kopp: Kidney Disease Section, National Instituteof Diabetes and Digestive and Kidney Diseases, National Institutesof Health, Building 10, 3N116, Bethesda, MD 20892.

References

Top
Author & Article Info
References

1. Rao TK, Filippone EJ, Nicastri AD, Landesman SH, Frank E, Chen CK, et al. Associated focal and segmental glomerulosclerosis in the acquired immunodeficiency syndrome N Engl J Med. 1984;310:669-73. [PMID: 6700641].[Abstract]

2. Pardo V, Aldana M, Colton RM, Fischl MA, Jaffe D, Moskowitz L, et al. Glomerular lesions in the acquired immunodeficiency syndrome Ann Intern Med. 1984;101:429-34. [PMID: 6476632].

3. Gardenswartz MH, Lerner CW, Seligson GR, Zabetakis PM, Rotterdam H, Tapper ML, et al. Renal disease in patients with AIDS: a clinicopathologic study Clin Nephrol. 1984;21:197-204. [PMID: 6733986].[Medline]

4. Kimmel PL. The nephropathies of HIV infection: pathogenesis and treatment Curr Opin Nephrol Hypertens. 2000;9:117-22. [PMID: 10757215].[Medline]

5. Rao TK, Friedman EA, Nicastri AD. The types of renal disease in the acquired immunodeficiency syndrome N Engl J Med. 1987;316:1062-8. [PMID: 3561458].[Abstract]

6. Rao TK. Acute renal failure syndromes in human immunodeficiency virus infection Semin Nephrol. 1998;18:378-95. [PMID: 9692351].[Medline]

7. Peraldi MN, Maslo C, Akposso K, Mougenot B, Rondeau E, Sraer JD. Acute renal failure in the course of HIV infection: a single-institution retrospective study of ninety-two patients anad sixty renal biopsies Nephrol Dial Transplant. 1999;14:1578-85. [PMID: 10383033].[Abstract/Free Full Text]

8. Perazella MA. Acute renal failure in HIV-infected patients: a brief review of common causes Am J Med Sci. 2000;319:385-91. [PMID: 10875295].[Medline]

9. Joshi MK, Liu HH. Acute rhabdomyolysis and renal failure in HIV-infected patients: risk factors, presentation, and pathophysiology AIDS Patient Care STDS. 2000;14:541-8. [PMID: 11054938].[Medline]

10. Kopp JB. Renal dysfunction in HIV-1-infected patients Curr Infect Dis Rep. 2002;4:449-460. [PMID: 12228033].[Medline]

11. Hare CB, Vu MP, Grunfeld C, Lampiris HW. Simvastatin-nelfinavir interaction implicated in rhabdomyolysis and death Clin Infect Dis. 2002;35:e111-2. [PMID: 12410494].[Medline]

12. Cheng CH, Miller C, Lowe C, Pearson VE. Rhabdomyolysis due to probable interaction between simvastatin and ritonavir Am J Health Syst Pharm. 2002;59:728-30. [PMID: 11977859].[Abstract/Free Full Text]

13. Castro JG, Gutierrez L. Rhabdomyolysis with acute renal failure probably related to the interaction of atorvastatin and delavirdine [Letter] Am J Med. 2002;112:505 [PMID: 11959068].[Medline]

14. Mastroianni CM, d'Ettorre G, Forcina G, Lichtner M, Corpolongo A, Coletta S, et al. Rhabdomyolysis after cerivastatin-gemfibrozil therapy in an HIV-infected patient with protease inhibitor-related hyperlipidemia [Letter] AIDS. 2001;15:820-1. [PMID: 11371708].[Medline]

15. Alpers CE. Light at the end of the TUNEL: HIV-associated thrombotic microangiopathy Kidney Int. 2003;63:385-96. [PMID: 12472814].[Medline]

16. Olyaei AJ, deMattos AM, Bennett WM. Renal toxicity of protease inhibitors Curr Opin Nephrol Hypertens. 2000;9:473-6. [PMID: 10990364].[Medline]

17. Krishnan M, Nair R, Haas M, Atta MG. Acute renal failure in an HIV-positive 50-year-old man Am J Kidney Dis. 2000;36:1075-8. [PMID: 11054370].[Medline]

18. Coca S, Perazella MA. Rapid communication: acute renal failure associated with tenofovir: evidence of drug-induced nephrotoxicity Am J Med Sci. 2002;324:342-4. [PMID: 12495304].[Medline]

19. Verhelst D, Monge M, Meynard JL, Fouqueray B, Mougenot B, Girard PM, et al. Fanconi syndrome and renal failure induced by tenofovir: a first case report Am J Kidney Dis. 2002;40:1331-3. [PMID: 12460055].[Medline]

20. Perazella MA. Crystal-induced acute renal failure Am J Med. 1999;106:459-65. [PMID: 10225250].[Medline]

21. Kopp JB, Miller KD, Mican JA, Feuerstein IM, Vaughan E, Baker C, et al. Crystalluria and urinary tract abnormalities associated with indinavir Ann Intern Med. 1997;127:119-25. [PMID: 9230000].[Abstract/Free Full Text]

22. Reilly RF, Tray K, Perazella MA. Indinavir nephropathy revisited: a pattern of insidious renal failure with identifiable risk factors Am J Kidney Dis. 2001;38:23 [PMID: 11576910].[Medline]

23. Engeler DS, John H, Rentsch KM, Ruef C, Oertle D, Suter S. Nelfinavir urinary stones J Urol. 2002;167:1384-5. [PMID: 11832739].[Medline]

24. Dieleman JP, van Rossum AM, Stricker BC, Sturkenboom MC, de Groot R, Telgt D, et al. Persistent leukocyturia and loss of renal function in a prospectively monitored cohort of HIV-infected patients treated with indinavir J Acquir Immune Defic Syndr. 2003;32:135-42. [PMID: 12571522].

25. Tokars JI, Frank M, Alter MJ, Arduino MJ. National surveillance of dialysis-associated diseases in the United States, 2000 Semin Dial. 2002;15:162-71. [PMID: 12100454].[Medline]

26. Eggers PW, Kimmel PL. Is there an epidemic of HIV nephropathy in the U.S ESRD program? [Abstract] J Am Soc Nephrol. 2002;12:38-A.

27. Weiner NJ, Goodman JW, Kimmel PL. The HIV-associated renal diseases: Current insight into pathogenesis and treatment Kidney Int. 2003;63:1618-31. [PMID: 12675837].[Medline]

28. Winston JA, Klotman PE. Are we missing an epidemic of HIV-associated nephropathy? [Editorial] J Am Soc Nephrol. 1996;7:1-7. [PMID: 8808103].[Abstract]

29. Szczech LA. Renal diseases associated with human immunodeficiency virus infection: epidemiology, clinical course, and management Clin Infect Dis. 2001;33:115-9. [PMID: 11389504].[Medline]

30. Kimmel PL, Umana WO, Bosch JP. Abnormal urinary protein excretion in HIV-infected patients Clin Nephrol. 1993;39:17-21. [PMID: 8428402].[Medline]

31. Hailemariam S, Walder M, Burger HR, Cathomas G, Mihatsch M, Binswanger U, et al. Renal pathology and premortem clinical presentation of Caucasian patients with AIDS: an autopsy study from the era prior to antiretroviral therapy Swiss Med Wkly. 2001;131:412-7. [PMID: 11571845].[Medline]

32. Szczech LA, Gange SJ, van der Horst C, Bartlett JA, Young M, Cohen MH, et al. Predictors of proteinuria and renal failure among women with HIV infection Kidney Int. 2002;61:195-202. [PMID: 11786101].[Medline]

33. Gardner LI, Holmberg SD, Williamson JM, Szczech LA, Carpenter CC, Rompalo AM, et al. Development of proteinuria or elevated serum creatinine and mortality in HIV-infected women J Acquir Immune Defic Syndr. 2003;32:203-9. [PMID: 12571531].

34. Mitra D, Kim J, MacLow C, Karsan A, Laurence J. Role of caspases 1 and 3 and Bcl-2-related molecules in endothelial cell apoptosis associated with thrombotic microangiopathies Am J Hematol. 1998;59:279-87. [PMID: 9840908].[Medline]

35. Eitner F, Cui Y, Hudkins KL, Schmidt A, Birkebak T, Agy MB, et al. Thrombotic microangiopathy in the HIV-2-infected macaque Am J Pathol. 1999;155:649-61. [PMID: 10433958].[Abstract/Free Full Text]

36. Hymes KB, Karpatkin S. Human immunodeficiency virus infection and thrombotic microangiopathy Semin Hematol. 1997;34:117-25. [PMID: 9109213].[Medline]

37. Park IW, Ullrich CK, Schoenberger E, Ganju RK, Groopman JE. HIV-1 Tat induces microvascular endothelial apoptosis through caspase activation J Immunol. 2001;167:2766-71. [PMID: 11509621].[Abstract/Free Full Text]

38. Sahud MA, Claster S, Liu L, Ero M, Harris K, Furlan M. von Willebrand factor-cleaving protease inhibitor in a patient with human immunodeficiency syndrome-associated thrombotic thrombocytopenic purpura Br J Haematol. 2002;116:909-11. [PMID: 11886400].[Medline]

39. Bottieau E, Colebunders R, Bosmans JL. Favourable outcome of haemolytic uraemic syndrome in an HIV-infected patient treated only with prednisone [Letter] J Infect. 2000;41:108-9. [PMID: 10942646].[Medline]

40. Sacristán Lista F, Saavedra Alonso AJ, Oliver Morales J, Vázquez Martul E. Nephrotic syndrome due to thrombotic microangiopathy (TMA) as the first manifestation of human immunodeficiency virus infection: recovery before antiretroviral therapy without specific treatment against TMA Clin Nephrol. 2001;55:404-7. [PMID: 11393387].[Medline]

41. Briggs WA, Tanawattanacharoen S, Choi MJ, Scheel PJ Jr, Nadasdy T, Racusen L. Clinicopathologic correlates of prednisone treatment of human immunodeficiency virus-associated nephropathy Am J Kidney Dis. 1996;28:618-21. [PMID: 8840956].[Medline]

42. Monga G, Mazzucco G, Boldorini R, Cristina S, Giacalone A, Fortunato M, et al. Renal changes in patients with acquired immunodeficiency syndrome: a post-mortem study on an unselected population in northwestern Italy Mod Pathol. 1997;10:159-67. [PMID: 9071721].[Medline]

43. Nochy D, Glotz D, Dosquet P, Pruna A, Guettier C, Weiss L, et al. Renal disease associated with HIV infection: a multicentric study of 60 patients from Paris hospitals Nephrol Dial Transplant. 1993;8:11-9. [PMID: 8381928].[Abstract/Free Full Text]

44. Kimmel PL, Ferreira-Centeno A, Farkas-Szallasi T, Abraham AA, Garrett CT. Viral DNA in microdissected renal biopsy tissue from HIV infected patients with nephrotic syndrome Kidney Int. 1993;43:1347-52. [PMID: 8315949].[Medline]

45. Casanova S, Mazzucco G, Barbiano di Belgiojoso G, Motta M, Boldorini R, Genderini A, et al. Pattern of glomerular involvement in human immunodeficiency virus-infected patients: an Italian study Am J Kidney Dis. 1995;26:446-53. [PMID: 7645552].[Medline]

46. Connolly JO, Weston CE, Hendry BM. HIV-associated renal disease in London hospitals QJM. 1995;88:627-34. [PMID: 7583076].

47. Praditpornsilpa K, Napathorn S, Yenrudi S, Wankrairot P, Tungsaga K, Sitprija V. Renal pathology and HIV infection in Thailand Am J Kidney Dis. 1999;33:282-6. [PMID: 10023639].[Medline]

48. Williams DI, Williams DJ, Williams IG, Unwin RJ, Griffiths MH, Miller RF. Presentation, pathology, and outcome of HIV associated renal disease in a specialist centre for HIV/AIDS Sex Transm Infect. 1998;74:179-84. [PMID: 9849552].[Abstract]

49. Kimmel PL, Phillips TM. Immune complex glomerulonephritis associated with HIV infection. In: Kimmel PL, Berns JS, Stein JH, eds. Renal and Urologic Aspects of HIV Infection. New York: Churchill Livingstone; 1995:77-110.

50. Chidambaram M, Stigant CE, Sugar LM, Ramesh Prasad GV. Type I membranoproliferative glomerulonephritis in an HIV-infected individual without hepatitis C co-infection Clin Nephrol. 2002;57:154-7. [PMID: 11865821].[Medline]

51. Alarcón-Zurita A, Salas A, Antón E, Morey A, Munar MA, Losada P, et al. Membranous glomerulonephritis with nephrotic syndrome in a HIV positive patient—remarkable remission with triple therapy [Letter] Nephrol Dial Transplant. 2000;15:1097-8. [PMID: 10862662].[Free Full Text]

52. Haas M, Rajaraman S, Ahuja T, Kittaka M, Cavallo T. Fibrillary/immunotactoid glomerulonephritis in HIV-positive patients: a report of three cases Nephrol Dial Transplant. 2000;15:1679-83. [PMID: 11007841].[Free Full Text]

53. Cheng JT, Anderson HL Jr, Markowitz GS, Appel GB, Pogue VA, D'Agati VD. Hepatitis C virus-associated glomerular disease in patients with human immunodeficiency virus coinfection J Am Soc Nephrol. 1999;10:1566-74. [PMID: 10405213].[Abstract/Free Full Text]

54. Stokes MB, Chawla H, Brody RI, Kumar A, Gertner R, Goldfarb DS, et al. Immune complex glomerulonephritis in patients coinfected with human immunodeficiency virus and hepatitis C virus Am J Kidney Dis. 1997;29:514-25. [PMID: 9100039].[Medline]

55. Guerra IL, Abraham AA, Kimmel PL, Sabnis SG, Antonovych TT. Nephrotic syndrome associated with chronic persistent hepatitis B in an HIV antibody positive patient Am J Kidney Dis. 1987;10:385-8. [PMID: 3674014].[Medline]

56. Korbet SM, Schwartz MM. Human immunodeficiency virus infection and nephrotic syndrome Am J Kidney Dis. 1992;20:97-103. [PMID: 1535750].[Medline]

57. Kimmel PL, Phillips TM, Ferreira-Centeno A, Farkas-Szallasi T, Abraham AA, Garrett CT. HIV-associated immune-mediated renal disease Kidney Int. 1993;44:1327-40. [PMID: 8301934].[Medline]

58. Katz A, Bargman JM, Miller DC, Guo JW, Ghali VS, Schoeneman MJ. IgA nephritis in HIV-positive patients: a new HIV-associated nephropathy? Clin Nephrol. 1992;38:61-8. [PMID: 1516281].[Medline]

59. Kimmel PL, Phillips TM, Ferreira-Centeno A, Farkas-Szallasi T, Abraham AA, Garrett CT. Brief report: idiotypic IgA nephropathy in patients with human immunodeficiency virus infection N Engl J Med. 1992;327:702-6. [PMID: 1495523].[Medline]

60. Beaufils H, Jouanneau C, Katlama C, Sazdovitch V, Hauw JJ. HIV-associated IgA nephropathy—a post-mortem study Nephrol Dial Transplant. 1995;10:35-8. [PMID: 7724026].[Abstract/Free Full Text]

61. Donadio JV, Grande JP. IgA nephropathy N Engl J Med. 2002;347:738-48. [PMID: 12213946].[Free Full Text]

62. Freedman BI, Soucie JM, Stone SM, Pegram S. Familial clustering of end-stage renal disease in blacks with HIV-associated nephropathy Am J Kidney Dis. 1999;34:254-8. [PMID: 10430971].[Medline]

63. Górriz JL, Rovira E, Sancho A, Ferrer R, Paricio A, Pallardó LM. IgA nephropathy associated with human immuno deficiency virus infection: antiproteinuric effect of captopril [Letter] Nephrol Dial Transplant. 1997;12:2796-7. [PMID: 9430904].[Free Full Text]

64. Boix E, Rivera F, Gil CM, Pérez-Contreras J, Olivares J. Steroid-responsive nephrotic syndrome with minimal-change disease and IgA deposits in a HIV-infected patient Nephrol Dial Transplant. 2000;15:412-4. [PMID: 10692530].[Free Full Text]

65. Mattana J, Siegal FP, Schwarzwald E, Molho L, Sankaran RT, Gooneratne R, et al. AIDS-associated membranous nephropathy with advanced renal failure: response to prednisone Am J Kidney Dis. 1997;30:116-9. [PMID: 9214410].[Medline]

66. Bourgoignie JJ. Renal complications of human immunodeficiency virus type 1 Kidney Int. 1990;37:1571-84. [PMID: 2194069].[Medline]

67. Klotman PE. HIV-associated nephropathy Kidney Int. 1999;56:1161-76. [PMID: 10469389].[Medline]

68. D'Agati V, Appel GB. HIV infection and the kidney J Am Soc Nephrol. 1997;8:138-52. [PMID: 9013459].[Abstract]

69. Winston JA, Klotman ME, Klotman PE. HIV-associated nephropathy is a late, not early, manifestation of HIV-1 infection Kidney Int. 1999;55:1036-40. [PMID: 10027941].[Medline]

70. Wali RK, Drachenberg CI, Papadimitriou JC, Keay S, Ramos E. HIV-1-associated nephropathy and response to highly-active antiretroviral therapy [Letter] Lancet. 1998;352:783-4. [PMID: 9737285].[Medline]

71. Levin ML, Palella F, Shah S, Lerma E, Butter J, Kanwar YS. Hiv-associated nephropathy occurring before HIV antibody seroconversion Am J Kidney Dis. 2001;37:39 [PMID: 11325704].[Medline]

72. Winston JA, Bruggeman LA, Ross MD, Jacobson J, Ross L, D'Agati VD, et al. Nephropathy and establishment of a renal reservoir of HIV type 1 during primary infection N Engl J Med. 2001;344:1979-84. [PMID: 11430327].[Free Full Text]

73. Cohen AH, Nast CC. HIV-associated nephropathy. A unique combined glomerular, tubular, and interstitial lesion Mod Pathol. 1988;1:87-97. [PMID: 3070550].[Medline]

74. D'Agati V, Appel GB. Renal pathology of human immunodeficiency virus infection Semin Nephrol. 1998;18:406-21. [PMID: 9692353].[Medline]

75. Strauss J, Abitbol C, Zilleruelo G, Scott G, Paredes A, Malaga S, et al. Renal disease in children with the acquired immunodeficiency syndrome N Engl J Med. 1989;321:625-30. [PMID: 2770791].[Abstract]

76. Kopp JB, Klotman ME, Adler SH, Bruggeman LA, Dickie P, Marinos NJ, et al. Progressive glomerulosclerosis and enhanced renal accumulation of basement membrane components in mice transgenic for human immunodeficiency virus type 1 genes Proc Natl Acad Sci U S A. 1992;89:1577-81. [PMID: 1542649].[Abstract/Free Full Text]

77. Reid W, Sadowska M, Denaro F, Rao S, Foulke J Jr, Hayes N, et al. An HIV-1 transgenic rat that develops HIV-related pathology and immunologic dysfunction Proc Natl Acad Sci U S A. 2001;98:9271-6. [PMID: 11481487].[Abstract/Free Full Text]

78. Alpers CE, Tsai CC, Hudkins KL, Cui Y, Kuller L, Benveniste RE, et al. Focal segmental glomerulosclerosis in primates infected with a simian immunodeficiency virus AIDS Res Hum Retroviruses. 1997;13:413-24. [PMID: 9075483].[Medline]

79. Stephens EB, Tian C, Dalton SB, Gattone VH 2nd. Simian-human immunodeficiency virus-associated nephropathy in macaques AIDS Res Hum Retroviruses. 2000;16:1295-306. [PMID: 10957726].[Medline]

80. Marras D, Bruggeman LA, Gao F, Tanji N, Mansukhani MM, Cara A, et al. Replication and compartmentalization of HIV-1 in kidney epithelium of patients with HIV-associated nephropathy Nat Med. 2002;8:522-6. [PMID: 11984599].[Medline]

81. Bruggeman LA, Ross MD, Tanji N, Cara A, Dikman S, Gordon RE, et al. Renal epithelium is a previously unrecognized site of HIV-1 infection J Am Soc Nephrol. 2000;11:2079-87. [PMID: 11053484].[Abstract/Free Full Text]

82. Ross MJ, Klotman PE. Recent progress in HIV-associated nephropathy J Am Soc Nephrol. 2002;13:2997-3004. [PMID: 12444220].[Free Full Text]

83. Bodi I, Abraham AA, Kimmel PL. Macrophages in HIV nephropathy Am J Kidney Dis. 1994;24:762-767.[Medline]

84. Segerer S, Nelson PJ, Schlöndorff D. Chemokines, chemokine receptors, and renal disease: from basic science to pathophysiologic and therapeutic studies J Am Soc Nephrol. 2000;11:152-76. [PMID: 10616852].[Abstract/Free Full Text]

85. Kinter A, Arthos J, Cicala C, Fauci AS. Chemokines, cytokines and HIV: a complex network of interactions that influence HIV pathogenesis Immunol Rev. 2000;177:88-98. [PMID: 11138789].[Medline]

86. Carrington M, Dean M, Martin MP, O'Brien SJ. Genetics of HIV-1 infection: chemokine receptor CCR5 polymorphism and its consequences Hum Mol Genet. 1999;8:1939-45. [PMID: 10469847].[Abstract/Free Full Text]

87. Conaldi PG, Biancone L, Bottelli A, Wade-Evans A, Racusen LC, Boccellino M, et al. HIV-1 kills renal tubular epithelial cells in vitro by triggering an apoptotic pathway involving caspase activation and Fas upregulation J Clin Invest. 1998;102:2041-9. [PMID: 9854039].[Medline]

88. Huber TB, Reinhardt HC, Exner M, Burger JA, Kerjaschki D, Saleem MA, et al. Expression of functional CCR and CXCR chemokine receptors in podocytes J Immunol. 2002;168:6244-52. [PMID: 12055238].[Abstract/Free Full Text]

89. Eitner F, Cui Y, Hudkins KL, Stokes MB, Segerer S, Mack M, et al. Chemokine receptor CCR5 and CXCR4 expression in HIV-associated kidney disease J Am Soc Nephrol. 2000;11:856-67. [PMID: 10770963].[Abstract/Free Full Text]

90. Bódi I, Kimmel PL, Abraham AA, Svetkey LP, Klotman PE, Kopp JB. Renal TGF-ß in HIV-associated kidney diseases Kidney Int. 1997;51:1568-77. [PMID: 9150474].[Medline]

91. Kimmel PL, Cohen DJ, Abraham AA, <