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Glomerular lesions in HIV-1-infected patients: evolution from 1996 to 2007 on 88 consecutive renal biopsies. Clara Flateau, François-Xavier Lescure, Emmanuelle.

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Presentation on theme: "Glomerular lesions in HIV-1-infected patients: evolution from 1996 to 2007 on 88 consecutive renal biopsies. Clara Flateau, François-Xavier Lescure, Emmanuelle."— Presentation transcript:

1 Glomerular lesions in HIV-1-infected patients: evolution from 1996 to 2007 on 88 consecutive renal biopsies. Clara Flateau, François-Xavier Lescure, Emmanuelle Plaisier, Patrice Callard, Jérôme Pacanowski, Pierre-Marie Girard, Pierre Ronco, Gilles Pialoux, for the ANAVIR study group.

2 Background 1984 : First description of HIV-associated nephropathy (HIVAN) Establishment of the direct pathogenic role of HIV-1 in HIVAN Identification of genetic suceptibility locus for HIVAN in Blacks (MYH9) (Kopp et al. 2008) HAART 1 : o Dramatic improvement of survival o Reduction in HIVAN incidence o Mild decrease in incidence of ESRD related to HIV HAART 2: o Nephrotoxicity of ARV agents o Comorbid conditions : diabetes, hypertension, aging, dyslipidemia = Risk factors for Chronic Kidney Diseases Lucas et al, AIDS, 2004

3 Method Aims – Describe the typological changes of glomerular disease in HIV-infected patients over study period (1996-2007) – Identify discriminant variables for HIVAN Design – Retrospective pathological study Data source – Pathology laboratory, Tenon Hospital, APHP – Departments of Infectious Diseases, Tenon and Saint Antoine Hospitals, APHP

4 Method Population – Consecutive adult HIV-infected patients with or without antiretroviral treatment – Kidney biopsies from 1995 to 2007 with diagnosis of glomerular disease Variables – Demographic variables – Hypertension, diabetes, dyslipidemia, history of cardiovascular events, and history of intravenous drug use. – Clinical data on HIV-infection, co-infections, CDC staging, history of opportunistic infections, ART history – Renal data including treatment, nephrotoxic drugs – Laboratory measurements at the time of biopsy

5 Method Kidney biopsies were analysed according to standard protocols Glomerular lesions were classified according to established criteria Glom Tub HIVAN Classical Focal and Segmental Glomerulosclerosis (FSGS)

6 Features of patients Total N= 88 1995-2000 N=27 2001-2003 N=29 2004-2007 N=32 p Median age, years [IQR]43 [34-50]38 [32-47]44 [34-53]46 [41-51]0.06 Men, n (%)69 (78.4)18 (66.7)21 (72.4)30 (93.8)0.03 Weight, kg [IQR]65 [58-72]63 [56-70]60 [53-67]72 [65-77]<0.01 Black, n (%)49 (71.0)18 (85.7)17 (77.3)14 (53.8)0.04 Undetectable HIV viral load, n (%)27 (37)6 (40)6 (21.4)15 (50)0.08 AIDS, n (%)45 (51.1)17 (63.0)15 (51.7)13 (40.6)0.23 ART, n (%)63 (71.6)17 (63.0)19 (65.5)27 (84.4)0.13 Hepatitis B, n (%)7 (8.9)1 (4.2)4 (15.4)2 (6.9)0.17 Hepatitis C, n (%)22 (26.2)7 (29.2)4 (14.3)11 (34.4)0.15 IDU n (%)9 (17.0)2 (22.2)3 (12.5)4 (20.0)0.72 Time HIV infection, months [IQR]84 [36-156]48 [24-114]108 [36-162]114 [36-171]0.04 CD4 count, cells/µL [IQR]217 [69-373]180 [15-354]211 [80-294]234 [143-449]0.18 GFR, ml/mn/1.73 m 2 [IQR]40 [12-63]20 [9-71]27 [11-52]55 [38-74]0.05 Proteinuria, mg/mmol [IQR]218 [114-508]406 [217-709]170 [108-400]160 [70-390]0.65

7 Features of patients Total N= 88 1995-2000 N=27 2001-2003 N=29 2004-2007 N=32 p Median age, years [IQR]43 [34-50]38 [32-47]44 [34-53]46 [41-51]0.06 Men, n (%)69 (78.4)18 (66.7)21 (72.4)30 (93.8)0.03 Weight, kg [IQR]65 [58-72]63 [56-70]60 [53-67]72 [65-77]<0.01 Black, n (%)49 (71.0)18 (85.7)17 (77.3)14 (53.8)0.04 Undetectable HIV viral load, n (%)27 (37)6 (40)6 (21.4)15 (50)0.08 AIDS, n (%)45 (51.1)17 (63.0)15 (51.7)13 (40.6)0.23 ART, n (%)63 (71.6)17 (63.0)19 (65.5)27 (84.4)0.13 Hepatitis B, n (%)7 (8.9)1 (4.2)4 (15.4)2 (6.9)0.17 Hepatitis C, n (%)22 (26.2)7 (29.2)4 (14.3)11 (34.4)0.15 IDU n (%)9 (17.0)2 (22.2)3 (12.5)4 (20.0)0.72 Time HIV infection, months [IQR]84 [36-156]48 [24-114]108 [36-162]114 [36-171]0.04 CD4 count, cells/µL [IQR]217 [69-373]180 [15-354]211 [80-294]234 [143-449]0.18 GFR, ml/mn/1.73 m 2 [IQR]40 [12-63]20 [9-71]27 [11-52]55 [38-74]0.05 Proteinuria, mg/mmol [IQR]218 [114-508]406 [217-709]170 [108-400]160 [70-390]0.65

8 History of patients Total N= 88 1995-2000 N=27 2001-2003 N=29 2004-2007 N=32 p ARV with potential nephrotoxicity Indinavir19 (22.4)3 (12.0)8 (27.6)8 (25.8)0.33 Atazanavir6 (7.1)006 (19.4)0.01 Lopinavir11 (13.9)04 (14.3)7 (28.0)0.01 Abacavir18 (22.8)1 (3.8)6 (21.4)11 (44.0)<0.01 Tenofovir15 (17.6)06 (20.7)9 (29.0)0.02 Hypertension, n (%)29 (33.0)8 (29.6)11 (37.9)10 (31.3)0.79 Diabetes mellitus, n (%)11 (12.6)4 (14.8)4 (13.8)3 (9.7)0.82 Dyslipidemia n (%)21 (24.1)4 (14.8)6 (21.4)11 (34.4)0.12 Lipodystrophy, n (%)6 (7.5%)03 (11.1%)3 (9.7%)0.28 History of cardiovascular events, n (%)6 (6.8)2 (7.4)2 (6.9)2 (6.3)0.98 ACE-I therapy n (%)14 (16.5)4 (16.0)3 (10.7)7 (21.9)0.51 ARBs therapy n (%)5 (6.0)02 (7.4)3 (9.4)0.31

9 History of patients Total N= 88 1995-2000 N=27 2001-2003 N=29 2004-2007 N=32 p ARV with potential nephrotoxicity Indinavir19 (22.4)3 (12.0)8 (27.6)8 (25.8)0.33 Atazanavir6 (7.1)006 (19.4)0.01 Lopinavir11 (13.9)04 (14.3)7 (28.0)0.01 Abacavir18 (22.8)1 (3.8)6 (21.4)11 (44.0)<0.01 Tenofovir15 (17.6)06 (20.7)9 (29.0)0.02 Hypertension, n (%)29 (33.0)8 (29.6)11 (37.9)10 (31.3)0.79 Diabetes mellitus, n (%)11 (12.6)4 (14.8)4 (13.8)3 (9.7)0.82 Dyslipidemia n (%)21 (24.1)4 (14.8)6 (21.4)11 (34.4)0.12 Lipodystrophy, n (%)6 (7.5%)03 (11.1%)3 (9.7%)0.28 History of cardiovascular events, n (%)6 (6.8)2 (7.4)2 (6.9)2 (6.3)0.98 ACE-I therapy n (%)14 (16.5)4 (16.0)3 (10.7)7 (21.9)0.51 ARBs therapy n (%)5 (6.0)02 (7.4)3 (9.4)0.31

10 Histologic glomerular lesions

11

12

13

14 Patients’ characteristics according to the type of FSGS HIVAN N=26 (%) Classical FSGS N=23 (%) OR (CI, 95%)p Mean age, years [IQR]40 [34-46]46 [38-53]/0.06 Men, n (%)20 (76.9)18 (78.3)1.1 (0.28-4.15)1.0 African American, n (%)22 (88.0)13 (68.4)0.3 (0.06-1.4)0.11 Time HIV infection, months [IQR]42 [8-96]108 [36-156]/0.03 CD4 count, cells/mm 3 [IQR]74 [22-185]367 [179-516]/<0.01 CD4<200/µL, n (%)21 (80.8)5 (23.8)0.07 (0.02-0.3)<0.01 Undetectable HIV viral load, n (%)4 (20.0)13 (61.9)6.5 (1.6-26.5)0.01 AIDS, n (%)11 (42)12 (52)0.5 (0.16-1.8)0.49 HAART, n (%)13 (50.0)21 (91.3)0.1 (0.02-0.5)<0.01 Hepatitis B, n (%)1 (4.3)1 (4.8)1.1 (0.06-18.8)0.75 Hepatitis C, n (%)2 (8.7)7 (31.8)4.9 (0.9-26.9)0.06

15 Patients’ characteristics according to the type of FSGS HIVAN N=26 (%) Classical FSGS N=23 (%) OR (CI, 95%)p Hypertension3 (12)11 (48)7.02 (1.6-30.1)<0.01 Dyslipidemia, n (%)3 (12)9 (39)4.7 (1.1-20.5)0.04 Diabetes mellitus, n (%)2 (8)2 (9)1.2 (0.15-9.3)0.86 Lipodystrophy, n (%)0 (0)3 (13.6)/0.09 GFR, ml/mn/1.73 m 2 [IQR]10 [7-26]52 [36-71]/<0.01 GFR<30 ml/mn/1.73 m2, n (%)24 (92.3)4 (17.4)0.02 (0.003-0.1)<0.01 Proteinuria, mg/mmol [IQR]215 [120-964]138 [104-420]/0.07

16 Risk factors associated with HIVAN Univariate analysisMultivariate analysis Risk factorsHIVAN n=26 Others n=62 OR (95% CI)p p African-Americans, n (%)22 (88)27 (61)4.6 (1.2-17.8)0.023.2 [0.5-21.6]0.2 CD4<200/mm 3, n (%)21 (81)18 (32)9.1 (3.0-28.0)<0.017.5 [1.4-39.7]0.02 GFR<30ml/mn/1.73m 2, n (%)24 (92)14 (23)41.1 (8.6-196)<0.0120.4 [3.5-120.3]<0.01 Absence of ARV, n (%)13 (50)12 (19)4.2 (1.5-11.3)<0.012.7 [0.6-12.8]0.2

17 HIVAN scale VariablesScore African-American origin3 points CD4<200/mm 3 8 points GFR<30ml/min/1.73m 2 20 points Absence of ARV3 points 1-specificity Sensitivity HIVAN scale > 21 points Sensitivity = 92% Specificity = 81% Positive predictive value = 67% Negative predictive value = 96% Area Under Curve = 0.93 (p<0.001) HIVAN scale > 21 points Sensitivity = 92% Specificity = 81% Positive predictive value = 67% Negative predictive value = 96% Area Under Curve = 0.93 (p<0.001) ROC curve

18 Discussion Less Blacks and HCV-coinfected patients than in prior African-American studies Indications for kidney biopsies could have changed between the 3 periods (under biopsy of HIVAN profile patients) A real switch of FSGS types over time Classical FSGS associated with long term infection, cardiovascular risk factors and lipodystrophy A discriminant clinical and biological scale for identification of HIVAN

19 Conclusion The emergence of one glomerular disease among treated HIV-infected patients: the classical FSGS A particular susceptibility for Black population concerning both main types of glomerular diseases in HIV infection, as previously shown in genetic linkage studies An HIVAN scale ≤ 21 points coud lead to perform the kidney biospy

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