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Current treatment of hepatitis C in HIV co-infected patients Dominique SALMON Internal Medicine Department, COCHIN Hospital Paris, FRANCE 12th ISVHLD - ANRS Co-infection day, July 5, 2006
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Main points Chronic HCV infection Candidates Pre therapeutic assessement Peg IFN and RBV doses Treatment duration Management of adverse events Acute HCV infection
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Candidates and Pretherapeutic assessement
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Candidates to therapy All HCV chronically infected patients should be offered treatment if the benefits outweigh the risks CD4 < 200/mm3 : treat HIV first Alcoholics : - same efficacy of PegIFN + RBV - Pb of adherence to treatment Active drug users: - opiate substitution priority - case by case evaluation Alberti et al, 1st ECC, J Hepatol 2005
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Pretherapeutic liver evaluation HCV genotype HCV viral load Liver biopsy: useful, but not mandatory when a decision to treat has been taken New markers of fibrosis
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Impact of genotype and HCV-RNA on SVR % pts with SVR in APRICOT Torriani et al NEJM 2004, 0 10 20 30 40 50 60 70 geno 1geno 2-3 > 5,9 log UI/ml < 5,9 log UI/ml
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Liver biopsy in HIV/HCV co- infected patients Genotype 1 and 4, and high HCV load (>800,000 IU/ml) Presence of co-morbidities : - Excessive alcohol consumption - HBV and/or delta co-infection - Medication hepatotoxicity Genotype 2 and 3 Genotype 1 and 4, and low HCV load (≤800,000 IU/ml) Required for treatment decision Not required for treatment decision Alberti et al, 1st ECC, J Hepatol 2005
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New tests of fibrosis FibroScan + seric markers Discordance Concordance Liver biopsy Treatment or follow-up Follow-up Minimal fibrosis < F2 Moderate or severe fibrosis F >2 Treatment Castera et al. Gastroenterology 2005; 128: 343-50.
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Doses of Peg IFN and ribavirin
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Doses of Peg-IFN ACTG 5071 RIBAVICLAGUNOAPRICOT Peg-IFN 2aPeg-IFN 2b Peg-IFN 2a 180 g/w Peg-IFN 2b 1.5 g/kg/w 40 27 44 0 20 40 60 80 100 SVR (%)
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SVR with PegIFN + RBV in HIV/HCV patients 38% (1 and 4) 14%17% (1 and 4) 29% Genotype 1 53%27%44%62% Genotype 2-3 44%27% 40%Gobal LAGUNORIBAVICACTG 5071 APRICOT
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Genotype 2 or 3 Genotype 1 or 4 Low ARN HCV < 800 000 UI/ml High ARN HCV > 800 000 UI/ml Ribavirin 800 mg Ribavirin 1000-1200 mg Alberti et al, 1st ECC, J Hepatol 2005 Dose of ribavirin is critical
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Genotype 2 or 3 Genotype 1 or 4 WhateverHIV-RNA Ribavirin 800 mg Ribavirin 1000-1200 mg Alberti et al, 1st ECC, J Hepatol 2005 Dose of ribavirinin 2006
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Increased ribavirine dose useful in genotype 1 with high viral load (WIN-R) Jacobson et al. LB3, AASLD 2005 Genotype 2, 3 65 58 68 60 0 70 24 weeks48 weeks SVR (%) 27 34 32 39 0 10 20 30 40 Viral load > 600 000 Ul/ml Viral load < 600 000 Ul/ml SVR (%) Genotype 1 p = 0.173 Group A: PEG-IFNα-2b + ribavirin 800 mg/d vs. Group B: PEG-IFNα-2b. + ribavirin 13 + 2 mg/kg G1: 48 weekG2-3 : 24 sem. vs. 48 week p = 0.047 725776446391322 316588602 n=
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PRESCO trial Study weeks 0 96 72 48 24 60 84 Peg-IFN + RBV 1000-1200 mg/day 12 36 Follow-up G2,3 G1,4 G2,3 Follow-up Only patients who achieved EVR (>2 log drop in HCV-RNA at week 12) continued treatment. n=389
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APRICOT (800mg/d) vs PRESCO and FRIED (1000-1200 mg/d) : genotype 1 response Soriano, ICAAC 2006, accepted On-treatment analysis 31% Percentage of patients 34% 29% 36% 46% 13% 0% 10% 20% 30% 40% 50% 60% 70% 80% 90% 100% <50UI/ml W4SVR Apricot Presco Fried
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Breilh D., Abstract 928, CROI 2005 RBV Concentration (mg/L) 0 0 0,5 1 1,5 2 2,5 3 3,5 1234567891011121314 Time (hours) D4W2W3 Virologic failure Virologic failure Virologic succes Virologic succes Relation between RBV concentration and sustained virologic response in Co-infected patients
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Recommended treatment duration = 48 weeks
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Positive predictive value of early virological response (EVR) on SVR 74 % 94% 58 % 82% 66 % 83% EVR at W4 > 2 log drop HCV RNA undetectable HCV-RNA 70 %45 %56 % EVR at W12 > 2 log drop HCV RNA Genotype 2/3 Genotype 1 All genotypes Torriani, NEJM, 2004, 292;
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Probability of success is evaluable as early as W4 >2 log HCV-RNA decrease HCV-RNA undetectable SVR probability 60% geno 1 58% SVR probability 83% geno 2/3 74%
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Negative predictive value of early virological response (EVR) 84 %90 %88 % No EVR at W4 < 2 log drop HCV RNA 100 %98 %- No EVR at W12 < 2 log drop HCV RNA Genotype 2/3 Genotype 1 All genotypes Torriani, NEJM, 2004, 292;
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Early viral Kinetics in RIBAVIC trial 82 94 71 99 0 20 40 60 80 100 W4W12 VPPVPN Carrat et al. JAMA 2004
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Duration of treatment Evaluate at week 12 early virological response HCV-RNA > 2 log Treatment for 48 weeks If HCV-RNA neg at W24 TTT should be stopped HCV-RNA < 2 log Alberti et al, 1st ECC, J Hepatol 2005
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Optimal duration for genotype 2,3 in HIV co-infected patients ?
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Keep patients on the optimal dose of peg-IFN and ribavirin Proactive management of adverse events and antiretroviral treatment 23%31%39%25%Tx interruption 31% pegIFN RBV 10% 25% 34% 18% 16% 20% 25% 18% dose AE Lab abnormality LagunoACTG 5071 RibavicApricot Torriani NEJM 2004;Carrat Jama 2004; Chung,NEJM 2004; Laguno AIDS 2004
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Impact of adherence on SVR with PegIFN a /ribavirin bitherapy SVR depends on RBV doses within the 12 first weeks Reddy et al. EASL 2005 p=0.01 66 57 45 0 0 10 20 30 40 50 60 70 >97%80-97%60-80%<60%
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Prevention and proactive management of adverse events betablockers levothyroxin Hyper or hyothyroidism No ddI (d4t) : RR X 2.3 Mitochondrial toxicity (1-3%) Liver decompensation avoid AZT Use EPO Use G-CSF Anemia Hb < 8 g/dl : 3.8% Neutropenia Manage depressive mood changes Depression paracetamol +/- NSAID Influenza-like syndrome keep > 95% of the dose mainly for the first 3 months
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RIBAVIC – Mitochondrial toxicity (pancreatitis –hyperlactatemia) Incidence –27,5 / 1000 pat./year (all) –34,1 / 1000 pat./year (with ARV) –0 / 1000 pat./year (without ARV) 2 %NoNon 0 %YesNo 7 %NoYes 24 %Yes % with mitochondrial toxicity d4TddI Multivariate analysis : odds-ratio for ddI = 23 [95 % CI : 5-105] Carrat et al. JAMA 2004; 292: 2839-2848
![RIBAVIC – Mitochondrial toxicity (pancreatitis –hyperlactatemia) Incidence –27,5 / 1000 pat./year (all) –34,1 / 1000 pat./year (with ARV) –0 / 1000 pat./year (without ARV) 2 %NoNon 0 %YesNo 7 %NoYes 24 %Yes % with mitochondrial toxicity d4TddI Multivariate analysis : odds-ratio for ddI = 23 [95 % CI : 5-105] Carrat et al.](http://images.slideplayer.com/25/7660659/slides/slide_29.jpg "JAMA 2004; 292:")
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AZT: impact on anemia and RBV doses 52 % 20 % 0 % 20 % 40 % 60 % AZTNo AZT Patients with RBV dose decrease Hb decrease at W4 3,14 1,96 0 1 2 3 AZTNo AZT Hb (g/dl) RBV dose decrease at W4 Alvarez D et al. 12th Conference on Retroviruses and Opportunistic Infections (Abstract #: P-192). Boston, MA USA, February 22–25, 2005
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*p = 0,009 ; † p < 0,001 ; ‡ p < 0,03 ; § p = 0,003 ; Epoetin alfa vs. Placebo. PhysicalMentalVitality † ‡ * § Afdhal et al. Gastroenterology 2004 Impact of Epoetin alfa 9% 5% 12% 14% 11% -1% 8% 9% 22% 6% 23% 25% -5 0 5 10 15 20 25 30 35 40 % Change from Study Entry Week9 17Week9 17Week9 17 Epoetin alfa / Placebo /Epoetin alfa
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Management of non responders Was the treatment adequate ? No Adherence Pb, side effects, low doses Yes 100% of the dose during the first 12 W Retreatment Partial response or relapse No response = true non responder
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Approach dependent on histology : Minimal disease => wait new drugs Significant disease (F3-F4) => –Monitor ESLD and HCC –Consider alternative strategies Maintenance therapy HAART Retreatment High dose peg-IFN? New drugs ?
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Acute HCV treatment
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Treatment of acute HCV hepatitis 168 HCV monoinfected: ALT (5-10x), PCR and/or sero-conversion Egypt, USA, Germany Geno 1, 4: 60% 1.5 g/kg/wk PEG 2b for 12 weeks Initiation from 1 st positive RNA result either at : SVR (%) Time of Rx onsetIntent to RxTreated 8 weeks (n=43)95%95% 12 weeks (n=43)93%91% 20 weeks (n=82)77%70% Kamal et al Gastroenterology 2006;130:632-8
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Treatment of acute HCV Kamal et al Gastroenterology 2006;130:632-8 Geno 1 Geno 2+3 Geno 4
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Comparison of the 2 largest studies of acute HCV infection Kamal et alWiegard et al N° patients16889 Rx duration12 weeks24 weeks SVR95% (early Rx)89% Main groupOcc exposure: 56%IDU, sex: 44% +ve factorsGeno non-1ALT >500 Kamal et al Gastroenterology 2006;130:632-8; Wiegand et al Hepatology 2006; 43: 250-6 PEG alone 12 weeks as good as 24 weeks Delay up to 12 weeks max from diagnosis Max chance of SVR for geno 2 or 3
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Treatment of acute HCV hepatitis in HIV infection N°RegimenDuration (weeks) genotype% SVR Vogel M et al 11Variable23-48GT 1/4 : 10 Other: 1 91% Gilleece YC et al 27PegIFN +RBV24GT 1: 20 Other : 4 55% 100% Dominguez S et al 14PegIFN + RBV24GT 1/4 : 8 Other: 3 71.4% Vogel et al, J Viral Hepatitis, 2005; Gilleece et al, J AIDS 2005;Dominguez S et al, submitted Initiation from PCR/seroconversion at 12 weeks
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Conclusion (1) As eradication is possible, hepatitis C treatment discussed for all patients, except if minimal liver disease Histological evaluation crucial: liver biopsy should not be an obstacle new tools available. Improved success rates with HCV therapy due to: –proactive management side effects –increased ribavirine dose (1000-1200mg genotype 1)
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Conclusion (2) Duration of treatment (48 weeks) depends on EVR: –at 12 weeks : stop if no significant response –at 24 weeks : stop if viral load remains positive. Fields of research : –Geno1, high VL : higher doses RBV and/or Peg IFN ? –Slow responders : longer duration of therapy ? –True non responders: maintenance therapy ? –New molecules.
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