Update on chronic hepatitis C treatment: current trends, new challenges, what next?

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1 Update on chronic hepatitis C treatment: current trends, new challenges, what next? Matti Maimets MMaimets15

2 Disclosure this presentation is sponsored by Gilead Sciences MMaimets15

3 MMaimets15 Science April 21,1989

4 The Fathers Houghton Nature Med 2000;6:1084 MMaimets15

5 MMaimets15 First Treatment Attempts

6 Interferon for chronic non-a, non-b hepatitis patients ALT levels fell to normal in 8, remained normal in 5 MMaimets15 Hoofnagle Paris 2012

7 MMaimets Pawlotsky ECCMID15

8 2010: The Directly Acting Antivirals (DAAs) MMaimets15

9 MMaimets14

10 MMaimets15 Hoofnagle Paris 2012

11 The DAAs PREVIRs ASVIRs BUVIRs MMaimets15 Schinazi Liver Int 2014;34:s69

12 previrs asvirs buvirs MMaimets15 Schinazi Liver Int 2014;34:s69

13 ,4 VIEKIRAX + EXVIERA HARVONI MMaimets15 Levero Paris 15

14 Current access to second-generation DAAs in the European region SMV SOF SMV PR SOF SOF/ LDV DCV 3D/r MMaimets15 As of April 21st, 2015; restrictions compared to EU label (fibrosis stage, genotype, treatment experience ) may apply, varying country by country Not showing early access programs Buti EASL 2015

15 The DAA regimens first-generation PI + PEG/RBV-based TLV + PEG/RBV BOC + PEG/RBV second-generation PI + PEG/RBV-based SOF + PEG/RBV SMV + PEG/RBV interferon free DAA combinations ± RBV MMaimets15

16 First-generation PI + PEG/RBV based regimens MMaimets15

17 MMaimets Pawlotsky ECCMID15

18 Adverse Events skin rash (TVR) anaemia leukopenia thrombopenia MMaimets15

19 Estonian NPP patients, 10 N, 12 M, G1b VL M F 1-2: 3, F 3: 15, F 4: 4 SVR24: 13/17 76% MMaimets15

20 Estonian NPP 2013 adverse events 20/22 skin: 10/22 anaemia: 9/22 stopped AE 1/22 manageable, but not without effort MMaimets15

21 MMaimets15

22 Sofosbuvir or Simeprevir + PEG/RBV based regimens MMaimets15

23 MMaimets

24 MMaimets15 Sofosbuvir + PR

25 N Eng J Med 2013;368 NEUTRINO STUDY MMaimets15

26 SVR12 (%) SOF + PR 12 weeks (NEUTRINO): SVR12 rates by HCV genotype in treatment-naïve patients / /292 27/28 7/7 Overall G1 G4 G5/6 mostly G1a Lawitz E, et al. EASL 2013; Oral presentation 1411

27 SOF + PR 12 weeks: impact of cirrhosis status and G1 subtype on efficacy in treatment-naïve patients (NEUTRINO) SVR12 (%) /180 36/43 47/56 6/9 Non-cirrhotic Cirrhotic Non-cirrhotic Cirrhotic G1a G1b FDA backgrounder for FDA advisory committee meeting; October 2013

28 Negative predictors: cirrhosis, IL289B non-cc, RNA > , BW < 75, male gender MMaimets15

29 MMaimets15 Simeprevir + PR

30 MMaimets15 Lancet 2014,384:403 & 414

31 SVR (%) Simeprevir + P/R: Phase III QUEST-1: Impact of Subtype & Fibrosis Stage in GT1 Overall GT1a GT1b F0-F2 F3 F Simeprevir P/R Simeprevir P/R SVR: GT1b > GT1a SVR: F0-F2 > F4 SVR is lowest for patients with GT1a and baseline Q80K mutation MMaimets15 Jacobson I, et al. EASL Abstract 1425.

32 Safety: The Major Advantage Regimen Trial HCV genotype/ population N F4 (% ) Grade 3 4 AE (%) SAEs D/C due to AEs(%) Notable AEs* Pooled SMV + PR 1 analysis Phase 2b/3 G1 TN & TE % 4 SOF + PR 2 Neutrino G1, 4-6 TN % 2 Increased bilirubin, rash Fatigue, headache, anemia, nausea, rash *Occurring more frequently vs PR except SOF/PR: most frequently reported AE in NEUTRINO. Lack of control arm did not allow identification of AEs occurring more frequently when SOF is added to PR D/C: discontinuations; TN: treatment naïve; TE: treatment experienced 1. Manns M, et al. Hep DART Poster Lawitz E, et al. N Engl J Med 2013;368: Hézode C, et al. AASLD Poster 755

33 What did these studies show 12W SOF + PR overall SVR12 90% 12W SMV + 24(48)W PR G1b SVR12 85% SVR depends on genotype 1b > 1a fibrosis stage, cirrhosis race BMI HCV RNA IU/ml IL28 subgroup safety is not an issue MMaimets15

34 2014: The Revolution Interferon free DAA combinations ± Ribavirin MMaimets15

35 MMaimets15

36 MMaimets15

37 MMaimets

38 MMaimets15 the most dramatic advance in treatment of an infectious disease since the discovery of penicillin

39 MMaimets15 Which DAAs Can Be Combined

40 Nukes 2 nd PI Non-nukes NS5A 1 st PI MMaimets15

41 J Med Virology early online Satoshi Yoshimi e.a. Long term persistence of NS5A inhibitor-resistant hepatitis C virus in patients who failed daclatasvir and asunaprevir therapy NS5A-L31M and -Y93H variants persisted as dominant strains until posttreatment week 170. MMaimets15

42 Studies of interferon free DAA combinations ± Ribavirin MMaimets15

43 LDV/SOF Clinical Development Program ELECTRON LONESTAR ELECTRON- 2 ION-2 ION-4 HCV/HIV Co-infection ERADICATE HCV/HIV Co-infection French ANRS HCV/HIV Co-infection Egypt GT 4 French GT 4,5 Russia GT 1,3 Korea/ Taiwan/ China GT 1 Australia TAP IVDU Japan GT 1 Nosocomial HCV SOLAR-1 SOLAR-2 ION-3 LONESTAR-3 SYNERGY Bleeding Disorders ION-1 SIRIUS Retreatment GT 1 GT 1, incl. PI failures GT 4 GT 1/4 GT 1/2/3/6 Immediate Post-liver Transplant GT 1/3 GT 4/5 Special populations Post-renal Transplant Brain Imaging Study Sickle Cell Anaemia 43

44 LDV/SOF Phase 3 Program LDV/SOF Phase 3 Program (ION-1, ION-2, ION-3) Wk 0 Wk 8 Wk 12 Wk 24 LDV/SOF + RBV ION-1 ION-2 LDV/SOF LDV/SOF + RBV LDV/SOF ION-3 LDV/SOF + RBV LDV/SOF ION-1: treatment naïve,16% cirrhotic; N = 865 ION-2: treatment experienced, 20% cirrhotic; N = 440 ION-3: treatment naïve, non-cirrhotic; N = 647 N = 1952 total patients (224 cirrhotics) Afdhal N, et al. N Engl J Med 2014; 370: ; Afdhal N, et al. N Engl J Med 2014;370: ; Kowdley K, et al. N Engl J Med 2014;370:

45 SVR12 (%) ION-1 (GT 1, Treatment-Naive, LDV/SOF±RBV x 12 or 24 weeks) SVR12 by Presence of Cirrhosis (ITT) 100 Absence of Cirrhosis Cirrhosis /180 32/34 178/184 33/33 181/184 31/33 179/181 36/36 LDV/SOF LDV/SOF + RBV LDV/SOF 12 Weeks 24 Weeks 97% (132/136) cirrhotic patients achieved SVR12 2 patients were lost to follow-up; 2 patients relapsed LDV/SOF + RBV Error bars represent 95% confidence intervals Sulkowski M, IAC 2014, LBPE16 45

46 MMaimets15 Levero Paris 15

47 MMaimets15 What did these studies show

48 Viirus Patsient MMaimets15 Levero Paris 15

49 Viirus Patsient RAV, MMaimets15 resistance associated variant (ravieelne quasispecies, Q80K) Levero Paris 15

50 Viirus Patsient RAV, MMaimets15 resistance associated variant (ravieelne quasispecies, Q80K) Levero Paris 15

51 MMaimets15 DDId

52 MMaimets15 HCV therapy

53 MMaimets15

54 MMaimets15

55 MMaimets15

56 MMaimets15 Guidelines 2015 G1,2,3

57 In Press, Corrected Proof, Available online 21 April 2015 MMaimets15

58 MMaimets15

59 MMaimets15

60 MMaimets15

61 G1, no or compensated cirrhosis AASLD/IDSA 2015 EASL 2015 BOC/TVR + PEG/RBV NR NR, it is possible, however SOF/RBV NR NR SOF/PEG/RBV NR 12W SIM/PEG/RBV naive, relaps NR 12/24W SIM/PEG/RBV partials, nulls NR 12/48W LDV/SOF naive 12W 8W, 12W, 12W + RBV LDV/SOF nulls 24W or 12W + RBV 24W + RBV SIM/SOF 24W ± RBV 24W or 12W + RBV DCV/SOF - 24W or 12W + RBV OBT/PTV/r/DSV G1a: 24W + RBV G1b: 12W + RBV G1a: 24W + RBV G1b: 12W + RBV MMaimets15

62 G1, decompensated cirrhosis AASLD/IDSA 2015 EASL 2015 BOC/TVR + PEG/RBV NR NR SOF/RBV NR NR SOF/PEG/RBV NR NR SIM/PEG/RBV NR NR LDV/SOF 24W or 12W + RBV 24W or 12W + RBV SIM/SOF NR NR DCV/SOF - 24W or 12W + RBV OBT/PTV/r/DSV NR NR MMaimets15

63 G2 & 3, no or compensated cirrhosis G2 AASLD/IDSA 2015 EASL 2015 SOF/RBV 12 16W 12W SOF/PEG/RBV 12W (PEG/RBV relapsers) 12W DCV/SOF - 12W G3 AASLD/IDSA 2015 EASL 2015 SOF/RBV 24W 24W (naives) SOF/PEG/RBV 12W 12W DCV/SOF - 12W + RBV MMaimets15

64 G2 & 3, decompensated cirrhosis G2 AASLD/IDSA 2015 EASL 2015 SOF/RBV 24 48W 16 20W SOF/PEG/RBV NR NR DCV/SOF - 24W or 12W + RBV G3 AASLD/IDSA 2015 EASL 2015 SOF/RBV 24 48W NR SOF/PEG/RBV NR NR DCV/SOF - 24W or 12W + RBV MMaimets15

65 MMaimets15 What s next

66 HCV ravimid 2015 INF-free + INF MMaimets15 Webster Lancet 2015;385:1124

67 MMaimets15 Clin Infect Dis June 2015

68 MMaimets15 Dore Clin Infect Dis 2015;60:1829

69 Perfectovir MMaimets15 Dore Clin Infect Dis 2015;60:1829

70 MMaimets15 Challenges

71 MMaimets15 Dore Clin Infect Dis 2015;60:1829

72 MMaimets15

73 MMaimets15

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