The kidneys in HIV infection - WordPress.com · THE KIDNEYS IN HIV INFECTION 3rd National AIDS...
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Dr Esther Tan Zhao Zhi
Department of Nephrology
Selayang Hospital
12th October 2014
THE KIDNEYS IN HIV INFECTION
3rd National AIDS Conference
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OUTLINE
• Diagnosis of Renal Disease in HIV patients
• Risk Factors for kidney disease in HIV patients
• Epidemiology and causes of kidney diseases in HIV patients
• HIVAN, HIVICKD, HIV ASSOCIATED THROMBOTIC MICROANGIOPATHY
• Antiretroviral treatment and potential side effects
• Renal replacement therapy in HIV patients
• Renal transplantation in HIV patients
• Management Strategies
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PREVALENCE OF HIV IN THE WORLD
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Mocroft A, Ledergerber B, Katlama C, et al. Decline in the AIDS and death rates in the EuroSIDA study: an observational study. THE LANCET • Vol 362 • July 5, 2003
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DIAGNOSIS OF RENAL DISEASE IN HIV PATIENTS
• AKIN
• RIFLE
• KDIGO AKI Guidelines 2012 AKI
• eGFR
• Serum Cystatin C
• Urine albumin to creatinine ratio / Urine protein to creatinine ratio
CKD
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DIAGNOSIS OF RENAL DISEASE IN HIV PATIENTS
• AKIN
• RIFLE
• KDIGO AKI Guidelines 2012
• eGFR
• Serum Cystatin C
• Urine albumin to creatinine ratio / Urine protein to creatinine ratio
CKD
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ACUTE KIDNEY INJURY
• Highly prevalent among HIV infected individuals particularly in those who have had AIDS-defining illness including opportunistic infection.
• Ten percent of patients experienced at least 1 episode of AKI over a 2-year period. (71 patients out of 754 patients)1
• More than half were attributed to underlying infections,
76% of which were AIDS-defining illness, and ~ 75% needed hospitalization.2.
1 Franceschini N, Napravnik S, Eron JJ Jr, Szczech LA, Finn WF. Incidence and etiology of acute renal failure among ambulatory HIV-infected patients. Kidney Int. 2005;67:1526–31.
2 Ando M, et al. How to manage HIV-infected patients with chronic kidney disease in the HAART era. Clin Exp Nephrol (2012) 16:363–372
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Franceschini N, Napravnik S, Eron JJ Jr, Szczech LA, Finn WF. Incidence and etiology of acute renal failure among ambulatory HIV-infected patients. Kidney Int. 2005;67:1526–31.
16:363–372
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Silva TI, Post FA, Griffin MD. HIV-1 Infection and the Kidney:An Evolving Challenge in HIV Medicine Mayo Clin Proc. September 2007;82(9):1103-1116.
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DIAGNOSIS OF RENAL DISEASE IN HIV PATIENTS
• AKIN
• RIFLE
• KDIGO AKI Guidelines 2012 AKI
• eGFR
• Serum Cystatin C
• Urine albumin to creatinine ratio / Urine protein to creatinine ratio
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MEASURING KIDNEY FUNCTION
• The Infectious Disease Society of America recommends that, at the time of HIV diagnosis:
• ALL patients should be assessed for evidence of CKD, and, if present, be appropriately staged for kidney disease. 1
• The best way to measure the GFR involves administering a foreign substance like inulin or radio-isotopes that the glomeruli will filter completely as waste, without reabsorption by the tubules, and measuring its clearance over time. 2
1 Kalyesubula R, Perazella MA. Nephrotoxicity of HAART. AIDS Research and Treatment Volume 2011, Article ID 562790 2 A. S. Levey, J. Coresh, K. Bolton et al., “K/DOQI clinical practice guidelines for chronic kidney disease: evaluation, classification, and stratification,” American Journal of Kidney Diseases, vol. 39, supplement 1, no. 2, pp. S1–S266, 2002
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MEASURING KIDNEY FUNCTION
Lucas GM, et al. Clinical Practice Guideline for the Management of Chronic Kidney Disease in Patients Infected With HIV: 2014 Update by the HIV Medicine Association of the Infectious Diseases Society of America. Clinical Infectious Diseases.
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• Studies found the CKD Epidemiology Collaboration (CKD-EPI) creatinine equation to be more accurate than the older Modification of Diet in Renal Disease (MDRD) equation in HIV-infected individuals. 1
• The CKD-EPI equation that uses both creatinine and cystatin C has been found to be somewhat more accurate and precise than equations based on a single biomarker in both the general population and in HIV-infected persons . 2,3,4
MEASURING KIDNEY FUNCTION
1 Levey AS, Stevens LA, Schmid CH, et al. A new equation to estimate glomerular filtration rate. Ann Intern Med 2009; 150:604–12. 2 Inker LA, Schmid CH, Tighiouart H, et al. Estimating glomerular filtration rate from serum creatinine and cystatin C. N Engl J Med 2012; 367:20–9. 3 Bhasin B, Lau B, Atta MG, et al. HIV viremia and T-cell activation differentially affect the performance of glomerular filtration rate equations based on creatinine and cystatin C. PLoS One 2013; 8: e82028. 4 Inker LA, Wyatt C, Creamer R, et al. Performance of creatinine and cystatin C GFR estimating equations in an HIV-positive population on antiretrovirals. J Acquir Immune Defic Syndr 2012; 61:302–9.
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WHY IS KIDNEY DISEASE IMPORTANT?
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Wyatt CM. Perspective The Kidney in HIV Infection: Beyond HIV-Associated Nephropathy Top Antiviral Med. 2012;20(3):106-110
• 17,235 patients
• Followup for 5.7 years
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• Observational Cohort Study
• 7 large HIV cohorts in UK – 20,132 patients
• Followup 5.3 years (median)
Ibrahim F, Hamzah L, Jones R, et al. Baseline Kidney Function as Predictor of Mortality and Kidney Disease Progression in HIV-Positive Patients. Am J Kidney Dis. 2012;60(4):539-547
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Ibrahim F, Hamzah L, Jones R, et al. Baseline Kidney Function as Predictor of Mortality and Kidney Disease Progression in HIV-Positive Patients. Am J Kidney Dis. 2012;60(4):539-547
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Waheed S, Matsushita K, Sang Y, et al. Combined Association of Albuminuria and Cystatin C–Based Estimated GFR With Mortality, Coronary Heart Disease, and Heart Failure Outcomes: The Atherosclerosis Risk in Communities (ARIC) Study. Am J Kidney Dis. 2012 August ; 60(2): 207–216
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Adapted from Clinical Practice Guideline for the Management of Chronic Kidney Disease in Patients Infected With HIV: 2014 Update by the HIV Medicine Association of the Infectious Diseases Society of America
CKD CLASSIFICATION Very high risk
High risk
Moderately increased risk
Low risk
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EPIDEMIOLOGY OF HIV INFECTION AND KIDNEY DISEASE
• In the USA, 1.5% (range 0.3–3.4%) of dialysis patients HIV infection 0.4% (range 0–1.0%) of dialysis patients AIDS.1
• However, as dialysis patients in the USA have not necessarily undergone routine screening for HIV infection since then, true incidence and prevalence estimates are probably higher than those reported. 2
• Black persons account for 10% of the general population in the USA but account for > 30% of patients with ESRD. 2
• Among persons with HIV infection who receive dialysis, 91% are Black.
1 Tokars JI, Frank M, Alter MJ, Arduino MJ. National surveillance of dialysis-associated disease in the United States, 2000. Semin Dial. 2002;15:162–71.
2 Ando M, et al. How to manage HIV-infected patients with chronic kidney disease in the HAART era. Clin Exp Nephrol (2012) 16:363–372
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Ando M, et al. How to manage HIV-infected patients with chronic kidney disease in the HAART era. Clin Exp Nephrol (2012) 16:363–372
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• The prevalence of CKD among the HIV seropositive patients in Sg Buloh Hospital was 9.47%.
CKD stage 1 (16 patients)
77.9%
CKD stage 2 (9 patients)
17.6%
CKD stage 3 (15 patients) 3%
CKD stage 4 (7 patients) 1.4%
CKD stage 5 (One patient)
0.2%
Abstract WCN 2013
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RISK FACTORS FOR KIDNEY DISEASE IN HIV PATIENTS
Adapted from Clinical Practice Guideline for the Management of Chronic Kidney Disease in Patients Infected With HIV: 2014 Update by the HIV Medicine Association of the Infectious Diseases Society of America
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CAUSES OF CKD IN HIV PATIENTS
Ando M, et al. How to manage HIV-infected patients with chronic kidney disease in the HAART era. Clin Exp Nephrol (2012) 16:363–372
Traditional HIV-specific glomerular
disease
HIVAN
HIVICKD
HIV-related TMA
Comorbidities
Hypertension
Diabetes Mellitus
Hepatitis C / Hepatitis B
Drugs
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HIV-SPECIFIC AND HIV NON-SPECIFIC GLOMERULAR DISEASES OBSERVED IN HIV-INFECTED PATIENTS
Diseases Clinical characteristics HIV-specific disease
HIVAN Detectable viral load, high amount of proteinuria, rapid progression of renal failure
HIVIC (HIV-associated immune complex kidney disease)
Proteinuria and/or haematuria, variable manifestation including AKI
TMA (Thrombotic microangiopathy)
AKI, proteinuria, haematuria with microangiopathic haemolytic anaemia and thrombocytopaenia
HIV nonspecific disease
HCV-related MPGN/cryoglobulinemia
Proteinuria and/or haematuria, nephritic syndrome, decrease in serum complements
Diabetic nephropathy Proteinuria (microalbuminuria to nephrotic syndrome), decrease in GFR
Glomerular sclerosis Older patients, hypertension, no or low amount of proteinuria, coexistence of atherosclerotic diseases
Membranous glomerulopathy Nephrotic syndrome, idiopathic and secondary causes associated with HBV or cancers
Minimal change disease Nephrotic syndrome, use of NSAIDs
IgA nephropathy Haematuria and/or proteinuria with or without renal failure
Postinfectious glomerulonephritis Haematuria and/or proteinuria with or without renal failure
Ando M, et al. How to manage HIV-infected patients with chronic kidney disease in the HAART era. Clin Exp Nephrol (2012) 16:363–372
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Figure comparing HIV-positive with HIV-negative patients biopsied during study period of 1 year (2003-2004 ) at Chris
Hani Baragwanath Hospital, South Africa.
Gerntholz TE, Goetsch SJW, Katz I. HIV-related nephropathy: A South African Perspective. Kidney International (2006) 69, 1885–1891
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COMORBIDITIES OF DIABETES, HYPERTENSION
• Diabetes and hypertension account for more than 70% of all ESRD in the general US population.1
• Aging of the HIV infected population and prolonged exposure to antiretroviral regimens promote the development of diabetes and hypertension2
• Diabetes and hypertension have also been identified as independent risk factors for CKD among HIV-infected individuals in Europe.3
1 United States Renal Data System (USRDS) 2011 Annual Data Report: Atlas of Chronic Kidney Disease and End-Stage Renal Disease in the United States. http://www.usrds.org/adr.htm 2011. 2 Mallipattu SK, Salem F, Wyatt CM. The changing epidemiology of HIV-related chronic kidney disease in the era of antiretroviral therapy. Kidney International (2014) 86, 259–265; 3 Mocroft A, Kirk O, Reiss P et al. Estimated glomerular filtration rate, chronic kidney disease and antiretroviral drug use in HIV-positive patients. AIDS 2010; 24: 1667–1678.
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HEPATITIS C CO-INFECTION
• An estimated 10 million individuals worldwide are coinfected with HIV and HCV.1
• Hepatitis C coinfection is associated with a significant increase in risk of CKD progression among HIV-infected individuals
• Metaanalysis. Wyatt CM, Malvestutto C, Coca SG et al. The impact of hepatitis C virus coinfection on HIV-related
kidney disease: a systematic review and metaanalysis. AIDS 2008; 22: 1799–1807.
• Women’s Interagency HIV Study. Tsui J, Vittinghoff E, Anastos K et al. Hepatitis C seropositivity
and kidney function decline among women with HIV: data from the Women’s Interagency HIV Study. Am J Kidney Dis 2009; 54: 43–50.
• Veterans’ Aging Cohort Study. Fischer MJ, Wyatt CM, Gordon K et al. Hepatitis C and the risk of
kidney disease and mortality in veterans with HIV. J Acquir Immune Defic Syndr 2010; 53: 222–226.
• EuroSIDA. Peters L, Grint D, Lundgren JD et al. Hepatitis C virus viremia increases the incidence of chronic kidney
disease in HIV-infected patients. AIDS 2012; 26: 1917–1926.
1 Mallipattu SK, Salem F, Wyatt CM. The changing epidemiology of HIV-related chronic kidney disease in the era of antiretroviral therapy. Kidney International (2014) 86, 259–265
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Traditional HIV-specific glomerular
disease
HIVAN
HIVICKD
HIV-related TMA
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HIV ASSOCIATED NEPHROPATHY
• First described in New York in 1984.1
• The estimated prevalence of HIVAN has ranged from 3.5% in clinical studies to 12% in autopsy studies.2
• Renal biopsy is the only means to establish the diagnosis of HIVAN.3
1 Rao TK, Filippone EJ, Nicastri AD et al. Associated focal and segmental glomerulosclerosis in the acquired immunodeficiency syndrome. N Engl J Med 1984; 310: 669–673. 2 Ahuja TS, Borucki M, Funtanilla M, Shahinian V, Hollander M, Rajaraman S. Is the prevalence of HIV-associated nephropathy decreasing? Am J Nephrol 1999; 19:655–9 3 Roling J, Schmid H, Fischereder M, et al. HIV-Associated Renal Diseases and Highly Active Antiretroviral Therapy-induced nephropathy. Clinical Infectious Diseases 2006; 42:1488–95
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Mallipattu SK, Salem F, Wyatt CM. The changing epidemiology of HIV-related chronic kidney disease in the era of antiretroviral therapy. Kidney International (2014) 86, 259–265
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Lucas GM, Eustace JA, Sozio S, Mentari EK, Appiah KA, Moore RD. Highly active antiretroviral therapy and the incidence of HIV-1–associated nephropathy: a 12-year cohort study. AIDS 2004; 18:541–6
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PATHOGENESIS OF HIVAN AND OTHER HIV-RELATED KIDNEY DISEASES
Pays E, et al.The molecular arms race between African trypanosomes and humans. Nature Reviews Microbiology 12, 575–584 (2014)
Single-nucleotide polymorphisms in the apolipoprotein L1 (APOL1) gene
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TREATMENT OF HIVAN
• HAART
* Diagnosis of HIVAN is an indication for antiretroviral therapy regardless of viral load.
• ACE inhibitors 1
1 Wei A, Burns GC, Williams BA, Mohammed NB, Visintainer P, Sivak SL. Long-term renal survival in HIV-associated nephropathy with angiotensin-converting enzyme inhibition. Kidney Int 2003; 64:1462–71.
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HIVAN TREATMENT WITH HAART D
ialy
sis
-fre
e S
urv
ival
(n=26)
No ARV P = (0.025)
ARV Treatment
(n=10)
1000 0 2000 3000
0.00
0.25
0.50
0.75
1.00
Time (days)
Hopkins Nephrology HIV Cohort
ARV Treatment of HIVAN:
Dialysis Free Survival Estimates Atta et al., Nephrol Dial Transpl, 2006
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HAART AND HIVAN INCIDENCE 12-YEAR COHORT STUDY
No AIDS AIDS
Cases p
er
1000 p
ers
on
-years
0
5
10
15
20
25
30
35
40
45
Lucas GM, et al. AIDS. 2004;20:18(3):541-546.
Numbers in bars represent point estimates for HIV-associated nephropathy incidence in cases per 1000 person-years. Brackets above bars represent upper limits of 95% confidence intervals.
No Antiretroviral Therapy
Nucleoside Reverse Transcriptase Inhibitor Therapy
Highly Active Antiretroviral Therapy
Presumed HIV-Associated Nephropathy Incidence Stratified by AIDS Status and
Antiretroviral Use
2.6 5.0
26.3
14.4
6.8 0.0
Risk of HIVAN low in
patients without AIDS
NO HIVAN when HAART
used without AIDS
occurrence
Lower HIVAN associated
with NRTI and HAART use
compared with no ART in
patients with AIDS
(p < 0.001 for trend)
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Traditional HIV-specific glomerular
disease
HIVAN
HIVICKD
HIV-related TMA
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HIV-ASSOCIATED IMMUNE COMPLEX KIDNEY DISEASE
• The prevalence of HIV-associated, immune complex–mediated glomerulonephritides has been estimated to be 15%–80%. 1
• May present as:
• postinfectious glomerulonephritis,
• membranous nephritis,
• IgA nephritis,
• fibrillary glomerulonephritis,
• immunotactoid glomerulopathy
• membranoproliferative glomerulonephritis
• lupus-like syndrome 2,3
1 Roling J, Schmid H, Fischereder M, et al. HIV-Associated Renal Diseases and Highly Active Antiretroviral Therapy-induced nephropathy. Clinical Infectious Diseases 2006; 42:1488–95 2 Kimmel PL, Barisoni L, Kopp JB. Pathogenesis and treatment of HIVassociated renal diseases: lessons from clinical and animal studies, molecular pathologic correlations, and genetic investigations. Ann Int Med 2003; 139:214–27. 3 Nochy D, Glotz D, Dosquet P, et al. Renal disease associated with HIV infection: a multicentric study of 60 patients from Paris hospitals. Nephrol Dial Transplant 1993; 8:11–9.
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TREATMENT OF HIV-ASSOCIATED IMMUNE COMPLEX KIDNEY DISEASE
• No RCT
• Seem to benefit from treatment with :
• ACE-inhibitors
• Glucocorticoids
• Antiretroviral therapy. 1,2
1 Tabechian D, Pattanaik D, Suresh U, Cohn SE, Nadasdy T. Lupuslike nephritis in an HIV-positive patient: report of a case and review of the literature. Clin Nephrol 2003; 60:187–94. 2 Gorriz JL, Rovira E, Sancho A, Ferrer R, Paricio A, Pallardo LM. IgA nephropathy associated with human immunodeficiency virus infection: antiproteinuric effect of captopril. Nephrol Dial Transplant 1997; 12:2796–7.
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Bruggeman LA, Nelson PJ. Controversies in the pathogenesis of HIV-associated renal diseases. Nat. Rev. Nephrol. 5, 574–581 (2009);
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Traditional HIV-specific glomerular
disease
HIVAN
HIVICKD
HIV-related TMA
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HIV-ASSOCIATED THROMBOTIC MICROANGIOPATHY
• Predominantly affects white populations, children and young males.1
• Compared with HIVAN, TMA is rare, but HIV-related TMA may account for up to 35% of all TMA cases. 2,3
• Occurs late in the course of HIV infection and its incidence has dropped markedly since the advent of antiretroviral therapy.
1 Novitzky N, Thomson J, Abrahams L, du Toit C, McDonald A. Thrombotic thrombocytopenic purpura in patients with retroviral infection is highly responsive to plasma infusion therapy. Br J Haematol. 2005;128(3):373-379. 2 Thompson CE, Damon LE, Ries CA, Linker CA. Thrombotic microangiopathies in the 1980s: clinical features, response to treatment, and the impact of the human immunodeficiency virus epidemic. Blood. 1992;80(8): 1890-1895. 3 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 and sixty renal biopsies. Nephrol Dial Transplant. 1999;14(6):1578-1585.
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HIV-ASSOCIATED THROMBOTIC MICROANGIOPATHY
• Haemolytic uraemic syndrome
• Microangiopathic anemia and renal impairment
• Thrombotic thrombocytopaenic purpura
• Microangiopathic anemia,
• Thrombocytopenia
• Renal impairment
• Fever
• Neurologic features
Silva TI, Post FA, Griffin MD. HIV-1 Infection and the Kidney:An Evolving Challenge in HIV Medicine Mayo Clin Proc. September 2007;82(9):1103-1116.
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HIV-ASSOCIATED THROMBOTIC MICROANGIOPATHY
• Pathogenesis unclear
• Probably due to endothelial injury caused by :
• exposure to circulating viral proteins, and / or
• many other factors including :
• medications,
• circulating proinflammatory molecules,
• antiphospholipid antibodies.
Ross MJ. Advances in the pathogenesis of HIV-associated kidney diseases. Kidney International (2014) 86, 259–265;
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HIV-ASSOCIATED THROMBOTIC MICROANGIOPATHY
• There are no clinical trials to guide the treatment of HIV-TMA.
• Treatment :
• plasma infusion and plasmapheresis,1
• Splenectomy reserved for refractory disease. 1
• Antiretroviral therapy.2
• Anectodal experience with corticosteroids, and vincristine.1
• Mortality exceeds 60% in HIV-associated TMA. 1
1 Silva TI, Post FA, Griffin MD. HIV-1 Infection and the Kidney:An Evolving Challenge in HIV Medicine Mayo Clin Proc. September 2007;82(9):1103-1116. 2 Ross MJ. Advances in the pathogenesis of HIV-associated kidney diseases. Kidney International (2014) 86, 259–265;
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IMPACT OF ANTIRETROVIRAL THERAPIES ON KIDNEY
FUNCTION
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REVERSE TRANSCRIPTASE INHIBITORS
• There are two main categories of reverse transcriptase inhibitors (RTI).
• Nucleoside (NRTI) and nucleotide (NtRTI) analogs,
• inhibit reverse transcription of viral RNA to DNA by becoming incorporated into the viral DNA termination of DNA chain elongation.
• Non-nucleoside RTI, do not become incorporated into viral DNA but directly binds to and inhibit reverse transcriptase function.
Ross MJ. Advances in the pathogenesis of HIV-associated kidney diseases. Kidney International (2014) 86, 259–265;
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NUCLEOSIDE REVERSE TRANSCRIPTASE INHIBITORS
• Nearly all NRTI capable of causing systemic lactic acidosis with the highest risk being associated with stavudine and didanosine.
• NRTI cause type B lactic acidosis by inhibiting function of DNA polymerase - ɣ reduced cellular mitochondrial DNA content reduced expression of proteins necessary for oxidative phosphorylation increased oxidative stress due to mitochondrial injury.
Ross MJ. Advances in the pathogenesis of HIV-associated kidney diseases. Kidney International (2014) 86, 259–265;
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NUCLEOSIDE REVERSE TRANSCRIPTASE INHIBITORS
• This mechanism of mitochondrial dysfunction in proximal tubular cells explains the association of stavudine and lamivudine with Fanconi syndrome.1
• Another report described acute kidney injury and biopsy proven interstitial nephritis after exposure to abacavir.2
1 Ross MJ. Advances in the pathogenesis of HIV-associated kidney diseases. Kidney International (2014) 86, 259–265 2 P. De Beaudrap, M. B. Diallo, R. Landman et al., “Changes in the renal function after tenofovir-containing antiretroviral therapy initiation in a Senegalese Cohort (ANRS 1215),” AIDS Research and Human Retroviruses, vol. 26, no. 11, pp. 1221–1227, 2010.
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NUCLEOTIDE REVERSE TRANSCRIPTASE INHIBITORS
• Adefovir and cidofovir, are approved for treatment of hepatitis B and cytomegalovirus, respectively.
• Adefovir, which is approved for use against hepatitis B, was initially developed as an anti-HIV medication, it was never approved for use because of nephrotoxicity when used at high dose (10-fold higher dose than for hep B) necessary for antiHIV efficacy.
• Tenofovir, adefovir and cidofovir are all capable of inducing renal tubular injury.
Ross MJ. Advances in the pathogenesis of HIV-associated kidney diseases. Kidney International (2014) 86, 259–265;
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Ross MJ. Advances in the pathogenesis of HIV-associated kidney diseases. Kidney International (2014) 86, 259–265; Tourret J, Deray G, Isnard-Bagnis C. Tenofovir Effect on the Kidneys of HIV-Infected Patients: A Double-Edged Sword? J Am Soc Nephrol 24: 1519–1527, 2013
• 0.7-10% of patients may develop tenofovir-induced AKI
• 22-81% may develop subclinical signs of tubulopathy hyperphosphaturia
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Ross MJ. Advances in the pathogenesis of HIV-associated kidney diseases. Kidney International (2014) 86, 259–265
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Tourret J, Deray G, Isnard-Bagnis C. Tenofovir Effect on the Kidneys of HIV-Infected Patients: A Double-Edged Sword? J Am Soc Nephrol 24: 1519–1527, 2013
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RISK FACTORS FOR TENOFOVIR INDUCED RENAL TOXICITY
• Background renal dysfunction
• African American ethnicity
• Female gender
• CD4+ nadir < 200 cells / mm3
• Concomitant nephrotoxic medications
• acyclovir, ganciclovir, cidofovir, aminoglycosides, pentamidine, amphotericin
• Comorbid conditions
• Diabetes, hypertension, co infection with Hep B/C
• Older age
1 N. Crum-Cianflone, A. Ganesan, N. Teneza-Mora et al., “Prevalence and factors associated with renal dysfunction among HIV-infected patients,” AIDS Patient Care and STDs, vol. 24, no. 6, pp. 353–360, 2010. 2 M. Nelson, A. Azwa, A. Sokwala, R. S. Harania, and J. Stebbing, “Fanconi syndrome and lactic acidosis associated with stavudine and lamivudine therapy,” AIDS, vol. 22, no. 11, pp. 1374–1376, 2008.
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HIV PROTEASE INHIBITORS
• Inhibit the ability of the viral protease to process Gag structural polyproteins inhibiting viral maturation, rendering virions noninfectious.
• Most protease inhibitors are poorly soluble in aqueous solution promote crystalluria and/or nephrolithiasis when concentrated in the urine.
Ross MJ. Advances in the pathogenesis of HIV-associated kidney diseases. Kidney International (2014) 86, 259–265
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HIV PROTEASE INHIBITORS
• Indinavir reported to be associated with :
• Nephrolithiasis
• AKI due to acute tubular obstruction by indinavir crystals and
• Chronic tubulointerstitial nephritis due to chronic occlusion of renal tubules by indinavir crystals.1
• The HIVMA-IDSA guidelines recommend that individuals receiving indinavir should drink at least 1.5 L of water per day and that periodic monitoring of creatinine and urinalysis for pyuria be performed in the first 6 months of treatment.2
1 Ross MJ. Advances in the pathogenesis of HIV-associated kidney diseases. Kidney International (2014) 86, 259–265 2 Silva TI, Post FA, Griffin MD. HIV-1 Infection and the Kidney:An Evolving Challenge in HIV Medicine Mayo Clin Proc. September 2007;82(9):1103-1116.
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NONNUCLEOSIDE REVERSE-TRANSCRIPTASE INHIBITORS
• Nevirapine, efavirenz, and delavirdine have been demonstrated to have a safe renal profile in controlled trials. 1
• A single case report linked efavirenz to renal toxicity on the basis of a hypersensitivity reaction involving pneumonitis, hepatitis, and interstitial nephritis.2
1 Roling J, Schmid H, Fischereder M et al. HIV-Associated Renal Diseases and Highly Active Antiretroviral Therapy–Induced Nephropathy. Clinical Infectious Diseases 2006; 42:1488–95 2 Angel-Moreno-Maroto A, Suarez-Castellano L, Hernandez-Cabrera M, Perez-Arellano JL. Severe efavirenz-induced hypersensitivity syndrome (not-DRESS) with acute renal failure. J Infect 2006; 52:e39–40.
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FUSION INHIBITORS
• Enfuvirtide has not been associated with severe renal adverse effects. 1
• In a safety analysis of 663 patients in the T-20 versus Optimized Regimen Only (TORO)–1 and TORO-2 trials, one patient who had a history of diabetes, proteinuria, and hematuria developed membranoproliferative glomerulonephritis.2
1 Roling J, Schmid H, Fischereder M et al. HIV-Associated Renal Diseases and Highly Active Antiretroviral Therapy–Induced Nephropathy. Clinical Infectious Diseases 2006; 42:1488–95 2 Lalezari JP, Henry K, O’Hearn M, et al. Enfuvirtide, an HIV-1 fusion inhibitor, for drug-resistant HIV infection in North and South America. N Engl J Med 2003; 348:2175–85.
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RENAL SYNDROMES ASSOCIATED WITH ANTIRETROVIRAL AGENTS
Type of Agent Drug(Trade Name) Clinical Syndrome
Nucleoside reverse transcriptase inhibitors
Abacavir Didanosine,Lamuvidine, Stavudine
AKI (AIN) Fanconi Sydrome
Nucleotide reverse transcriptase inhibitors
Tenofovir fumarate Fanconi syndrome, Nephrogenic DI, AKI (prox tubule damage)
Other reverse transcriptase inhibitors
Delavirdine Efavirenz Nevarapine
Protease inhibitors Indinavir Nelfinavir Ritonavir
Renal colic,urolithiasis, obstructive uropathy, AKI and CKD from interstitial nephritis and crystallisation Renal colic AKI
HIV-1 fusion inhibitor Enfurvirtide Membranoproliferative GN
Daugas E etal,KI 2005;67:393-403
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Scherzer R, et al. Association of Tenofovir Exposure with Kidney Disease Risk in HIV Infection. AIDS. 2012 April 24; 26(7): 867–875
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METABOLIC ALTERATIONS ASSOCIATED WITH ANTIRETROVIRAL TREATMENT
• Metabolic alterations associated with HAART may cause :
• Significant elevations in serum lipid levels 1
• Increase in diabetic renal disease
• Increase in hypertensive renal disease as well as vascular complications.
• A controlled study evaluated 1689 patients demonstrated a 4-fold risk of developing diabetes.
1 Roling J, Schmid H, Fischereder M et al. HIV-Associated Renal Diseases and Highly Active Antiretroviral Therapy–Induced Nephropathy. Clinical Infectious Diseases 2006; 42:1488–95 2 Brown TT, Cole SR, Li X, et al. Antiretroviral therapy and the prevalence and incidence of diabetes mellitus in the multicenter AIDS cohort study. Arch Intern Med 2005; 165:1179–84.
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METABOLIC ALTERATIONS ASSOCIATED WITH ANTIRETROVIRAL TREATMENT
• A cohort study (5578 patients) during 1984–2003 incidence of hypertension in 7.3% HIV patients incidence began to increase significantly after 2 years of antiretroviral therapy.
• The risk of developing hypertension was maximally elevated (OR, 1.7) after > 5 years of treatment with HAART, compared with the risk among HIV infected patients who did not receive treatment (OR, 0.79).
Seaberg EC, Munoz A, Lu M, et al. Association between highly active antiretroviral therapy and hypertension in a large cohort of men followed from 1984 to 2003. AIDS 2005; 19:953–60.
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RENAL REPLACEMENT THERAPY IN HIV-INFECTED INDIVIDUALS
• Hemodialysis
• Peritoneal dialysis
• Kidney transplantation
• Survival rates with HD and PD are very similar.
• For patients on dialysis, antiretroviral drug regimens and doses should be carefully reviewed and adjusted if necessary.
Wyatt CM. Perspective The Kidney in HIV Infection: Beyond HIV-Associated Nephropathy Top Antiviral Med. 2012;20(3):106-110
Options for managing ESRD in HIV patients
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SURVIVAL OF HIV-INFECTED PATIENTS RECEIVING RENAL REPLACEMENT
THERAPY
• IMPROVED and the mortality rate is now approaching that for ESRD in the general population.1
• A recent study reported survival rates at :
• 1 year for HIV-infected patients on dialysis of 95.2%
• 3 years – 71.7%
• 5 years – 62.7% 2
1 Ahuja TS, Grady J, Khan S. Changing trends in the survival of dialysis patients with human immunodeficiency virus in the United States. J Am Soc Nephrol 2002; 13: 1889–1893. 2 Trulla`s JC, Barril G, Cofan F et al. Outcome and Prognostic Factors in HIV-1-Infected Dialysis Patients in Spain in the HAART Era: A Case-Control GESIDA/SEN Study. 17th CROI (Conference on Retroviruses and Opportunistic Infections, San Francisco, 2010. Abstract 739.
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SURVIVAL OF HIV-INFECTED PATIENTS RECEIVING RENAL REPLACEMENT
THERAPY
• The risk factors for mortality in the HIV infected dialysis population :
• a lower CD4+ T-cell count,
• a higher viral load,
• the absence of antiretroviral therapy, and
• a history of opportunistic infections. 1,2,3
1 Trulla`s JC, Barril G, Cofan F et al. Outcome and Prognostic Factors in HIV-1-Infected Dialysis Patients in Spain in the HAART Era: A Case-Control GESIDA/SEN Study. 17th CROI (Conference on Retroviruses and Opportunistic Infections, San Francisco, 2010. Abstract 739. 2 Rodriguez RA, Mendelson M, O’Hare AM et al. Determinants of survival among HIV-infected chronic dialysis patients. J Am Soc Nephrol 2003; 14: 1307–1313. 3 Tourret J, Tostivint I, du Montcel ST et al. Outcome and prognosis factorsin HIV-infected hemodialysis patients. Clin J Am Soc Nephrol 2006; 1:1241–1247.
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Trullas JC, Cofan F, Tuset M, et al. Renal transplantation in HIV-infected patients: 2010 update. Kidney International (2011) 79, 825–842
RENAL TRANSPLANTATION IN HIV PATIENTS
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MANAGEMENT STRATEGIES
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Qualitative assessment for risk of kidney disease
• Race
• Family history of kidney disease
• CD4+ lymphocyte count
• HIV-1 RNA level
• History of use of nephrotoxic medications
• Comorbidities
• Diabetes mellitus
• Hypertension
• Hepatitis C coinfection
Screening studies at initial HIV documentation
• Urine analysis (for proteinuria)
• Serum creatinine (estimate creatinine clearance or glomerular filtration rate using appropriate formula)
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Abnormal values
- Grade ≥ 1+ proteinuria by dipstick
- Cr clearance or GFR < 60mls/min/1.73m2
- Evaluate proteinuria further with spot urine protein/creatinine ratio
- Perform renal ultrasound
- Consider referral to a nephrologist for further evaluation and
potentially biopsy.
IDSA guidelines 2005
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No abnormal values
Groups without risk factors for kidney disease should be
followed clinically and reassessed based on the occurrence of signs and symptoms or as clinical
events dictate.
Groups at risk for development of chronic kidney
disease should be rescreened annually.
*Patients on
tenofovir may require monitoring
every 3 months
• Individuals of African American race
• Individuals with diabetes, hypertension or Hep C coinfection
• Individuals with CD4+ counts < 200 cells/mm3
• Individuals with HIV RNA levels > 4000 copies/ml.
IDSA guidelines 2005
GROUPS AT RISK
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TAKE HOME MESSAGES
• Renal pathology in HIV-infected persons can be caused by a variety of mechanisms leading to a broad spectrum of clinical disease.
• Long-term survival contributes to an increase in HAART-induced metabolic alterations, diabetes, and hypertension and is likely to be associated with an increase in secondary renal damage, such as hypertensive nephrosclerosis and diabetic glomerulopathy.
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TAKE HOME MESSAGES
• HAART and other medical therapies for HIV-related infections have been associated with both short- and long-term toxicities including nephrotoxicity.
• Kidney abnormalities tend to develop in the setting of multiple treatments and cannot be always attributed to a specific drug.
• Renal function should therefore be monitored on a regular basis in patients with HIV receiving any antiretroviral agent.
• Early detection of risk factors, systematic screening for chronic causes of CKD, and appropriate referrals for kidney disease management should be advocated for improved patient care.
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THANK YOU