W5 HIV, HCV, and HBV Co-Infection Jayaweera

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1 HIV, HCV and HBV COINFECTION Dushyantha Jayaweera, M.D., M.R.C.O.G., F.A.C.P. Professor in Clinical Medicine Division of Infectious Diseases University of Miami Miller School of Medicine

Transcript of W5 HIV, HCV, and HBV Co-Infection Jayaweera

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HIV, HCV and HBV COINFECTION

Dushyantha Jayaweera, M.D., M.R.C.O.G., F.A.C.P.

Professor in Clinical Medicine

Division of Infectious Diseases

University of Miami Miller School of Medicine

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● Epidemiology

● Hepatitis C Virus natural History

● HCV/HIV Co-infection

● Novel drug therapies

● HBV infection

● HBV vaccinations

Outline

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

HCV Prevalence by Selected Groups in the United States

Hemophilia

Injecting Drug Users

Surgeons

Hemodialysis

Average Proportion Anti-HCV Positive (%)

General Population Adults

Military Personnel

STD Clients

Pregnant Women

Centers for Disease Control and Prevention, 2003.

87

79

10

6

3.5

2

1

0.3

0 10 20 30 40 50 60 70 80 90 100

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

Infectious Disease Burden Among Released Inmates: United States 1997

Infection/Disease Infected Inmates Released[1]

Total Infected in US Population

% of Total Infected

Population[1] HCV (anti-HCV+) 1,321,781-1,943,796 4,500,000*[2] 29.4-43.2

HIV 150,950–196,555 750,000† 20.1-26.2

TB 12,531 31,660† 39.6

1. Hammett TM, et al. Am J Public Health. 2002;92:1789-1794. 2. McQuillan GM, et al. In: Rizzetto M, et al, editors. Viral hepatitis and liver disease. Turin, Italy: Edizioni Minerva Medica; 1997. p. 267-270.

*Data based on prevalence estimate.†Centers for Disease Control and Prevention estimate.

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● Epidemiology

● Hepatitis C Virus natural History

● Pathogenesis of HCV

● HCV/HIV Co-infection

● Novel drug therapies

● HBV infection

● HBV vaccinations

Outline

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

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clinicaloptions.com/hepatitisHighlights from AASLD 2009

Worldwide Distribution of HCV Genotypes

Zein N. Clin Microbiol Rev. 2000;13:223-235. Reproduced with permission. http://cmr.asm.org/cgi/content/full/13/2/223?view=long&pmid=10755999.

1a1b234567-8-9Others

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

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● Epidemiology

● Hepatitis C Virus natural History

● HCV/HIV Co-infection

● Novel drug therapies

● HBV infection

● HBV vaccinations

Outline

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Liver-related Mortality UK Hemophiliac Cohort

• Liver deaths– HIV - 16.7-fold– HIV + 94.4-fold

• Risk after 10 years

Darby et al. Lancet. 1997;350:1425-1431.

0

20

40

60

80

100

HIV+ HIV- Generalpopulation

Liv

er

de

ath

s (

O/E

)

O/E, observed to expected ratio; UK, United Kingdom.

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Increased Risk of Cirrhosis and ESLD in HIV/HCV Coinfected

Patients

Graham et al. Clin Infect Dis. 2001;33:562-569.

Histological Cirrhosis Decompensated Liver Disease

Combined

Benhamou

Pol

Soto

Makris

Makris

Telfer

Eyster

Lesens

Combined

10.832.071.0.76

Relative Risk (95% CI)

.61 1.0 6.14 10 175.32

CI, confidence interval; ESLD, end stage liver disease; HCV, hepatitis C virus; HIV, human immunodeficiency virus.

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HIV/HCV Coinfection TrialsPEG IFN/RBV

PEG IFN alfa-2a 180 µg + RBV 600 mg 1 g/dIFN alfa-2a 6 MIU 3 MIU + RBV 600 mg 1 g/d

ACTG 5071USA(N = 133)

PEG IFN alfa-2a 180 µg + RBV 800 mgIFN alfa-2a 3 MIU + RBV 800 mgPEG IFN alfa-2a 180 µg + RBV placebo 800 mg

APRICOTInternational(N = 868)

PEG IFN alfa-2b 1.5 μg/kg + RBV 800 mg

IFN alfa-2b 3 MIU + RBV 800 mg

RIBAVICFrance(N = 412)

Treatment RegimenStudy

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

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APRICOTVirologic Response*–End of Treatment vs End of Follow-

up (Genotype 1)

*Defined as <50 IU/mL HCV RNA.Torriani et al. 11th CROI; February 8-11, 2004; San Francisco, Calif. Abstract 112.

8

21

38

7

14

29

0

10

20

30

40

50

60

Res

po

nse

(%

)

IFN alfa-2a/RBV PEG IFN alfa-2a/Placebo

PEG IFN alfa-2a/RBV

EOT EOTSVR SVR SVREOT

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APRICOTVirologic Response*–End of

Treatment vs End of Follow-up (Genotype 2 and 3)

*Defined as <50 IU/mL HCV RNA.

Torriani et al. 11th CROI; February 8-11, 2004; San Francisco, Calif. Abstract 112.

57

27

64

36

20

62

0

10

20

30

40

50

60

70

Res

po

nse

(%

)

IFN alfa-2a/RBV PEG IFN alfa-2a/Placebo

PEG IFN alfa-2a/RBV

EOT SVR EOT SVR EOT SVR

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● Epidemiology

● Hepatitis C Virus natural History

● HCV/HIV Co-infection

● Novel drug therapies (in mono infection with HCV)

● HBV infection

● HBV vaccinations

Outline

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clinicaloptions.com/hepatitisSmoother Waters Ahead? New Directions in the Management of HCV

HCV Lifecycle and STAT-C Targets

Adapted from Manns MP, et al. Nat Rev Drug Discov. 2007;6:991-1000.

Receptor bindingand endocytosis

Fusion and

uncoating

Transportand release

(+) RNA

Translation and

polyprotein processing

RNA replication

Virionassembly

Membranousweb

ER lumen

LD

LDER lumen

LD

NS3/4 protease inhibitors

NS5B polymerase inhibitors

*Role in HCV lifecycle not well defined

NS5A* inhibitors

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

On-Treatment Viral Kinetics

STAT-C drugs may improve both first and second phase kinetics

Second phase

First phase

HC

V R

NA

0 12 24 36 484

HCV RNA negative in blood

Wks

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Resistant Variants occurs Naturally

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Maximize Response and Minimize Resistance

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

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clinicaloptions.com/hepatitisAASLD Practice Guidelines: An Update

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● Epidemiology

● Hepatitis C Virus natural History

● HCV/HIV Co-infection

● Novel drug therapies (in mono infection with HCV)

● HBV infection

● HBV vaccinations

Outline

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Geographic Prevalence of Chronic Hepatitis B May Geographic Prevalence of Chronic Hepatitis B May Be Impacted by MigrationBe Impacted by Migration

World Health Organization. Geographic Prevalence of HBsAg. Data from 1996 (unpublished). http://www.who.int/vaccines-surveillance/graphics/htmls/hepbprev.htm. Accessed: June 14, 2007

2002 Yearbook of Immigration Statistics. http://uscis.gov/graphics/shared/aboutus/statistics/IMM02yrbk/IMM2002list.htm. Accessed: June 14, 2007.

Mahoney FJ. Clin Microbiol Rev. 1999;12:351-366.

HBsAg Prevalence

8% - High

2-7% - Intermediate

<2% - Low

Immigration numbers summed by continent from 1996-2002

~2 million Asians

~400,000South Americans

~350,000 Africans

~930, 000 Europeans

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Clinical Liver Disease and HBV Clinical Liver Disease and HBV GenotypeGenotype

Duong TN, et al. Journal of Medical Virology. 2004;72:551–557.

Diagnosis, n (%)

Genotypes N Asymptomatic carrier

Chronic hepatitis

Liver cirrhosis

HCC

Genotype A 11 8 (72.7) 3 (27.3) 0 0

Genotype B 14 10 (71.4) 3 (21.4) 0 1 (7.2)

Genotype C 350 129 (36.8) 126 (36.0) 50 (14.3) 45 (12.9)

Genotype D 38 32 (84.2)b 6 (15.8)a 0 0a

a P<0.05 vs genotype C.b P<0.001 vs genotype C.

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Is HBsAg present?Is HBsAg present?

Is IgM anti-HBc present?Is IgM anti-HBc present?

Is HBeAg or HBV DNA present?Is HBeAg or HBV DNA present? Is anti-HBs present?Is anti-HBs present?

Chronic Chronic HepatitisHepatitis

Acute Acute HepatitisHepatitis

Replicative HBV Replicative HBV infectioninfection

Non-replicative HBV Non-replicative HBV infectioninfection

Recovered or Recovered or vaccinated vaccinated

+/- anti-HBc+/- anti-HBc

No HBV No HBV infectioninfection

NoNo

YesYes

YesYes

YesYes

YesYes

NoNo

NoNoNoNo

Anti-HBc Anti-HBc +/-+/-

nonoyesyes

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To reduce the risk for transmission, HBsAg-To reduce the risk for transmission, HBsAg-positive persons should:positive persons should:

• Use condoms to protect nonimmune sex partners. • Refrain from donating blood, plasma, tissue, or semen. • HBsAg-positive pregnant women should be advised

their newborns to receive hepatitis B vaccine and hepatitis B immune globulin

• To protect the liver HBsAg-positive persons should be advised to avoid or limit alcohol consumption, vaccination against hepatitis A.

• 15%--25% of persons with chronic HBV infection are at risk for premature death from cirrhosis and liver cancer,

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Treatment of HBV in HIVTreatment of HBV in HIV

• Always start with emtricitabine/tenofovir • If the patient has been on lamivudine add

tenofovir• If the patient is on Epzicom change to

emtricitabine/tenofovir• If the patient has renal failure or low GFR <60

it is safer to use lamivudine or emtricitabine with entecavir than using dose adjusted emtricitabine/tenofovir

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Add another drug

without cross resistance

Monitor every 3 months

Addanother drug

orContinue

Monitor every 3 months

Continue Monitor every 6 months

Management Roadmap According to 24 Week Virologic Response

Inadequate response>104 copies/mL

Complete response <300 copies/mL

Partial response 300-104 copies/mL

Week 24: Early predictors of efficacy

Keeffe et al. Clin Gastroenterol Hepatol, 2007

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Monitoring for Drug Resistance

All patients • HBV DNA and ALT at baseline and at 3 months

after starting therapy (assess antiviral efficacy)

Mild liver disease• HBV DNA and ALT q 6 mo for first 2 years;

thereafter q 3 mo and at any change in therapy

Advanced liver disease/cirrhosis• HBV DNA and ALT q 3 mo with clinical evaluation

Locarnini S, et al. Antiviral Ther. 2004;9:679-693.

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Yang H, et al. Hepatology. 2003;38:705A. Lai CL, et al. Hepatology. 2003;38:262A.

V173L L180M A181V A184G S202I M204I M204V N236T M250V

Lamivudine

Entecavir

Telbivudine

Emtricitabine

Adefovir

YMDD

Cross Resistance with HBV Drugs

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Hepatitis B VirusWild Type and Mutants

• Wild type– Usual HBeAg (+) hepatitis

• Precore mutation (27% U.S. patients)1

– Abolishes HBeAg production• Core promoter mutation (44% U.S. patients)1

– Down-regulates HBeAg production• Treatment-induced mutations2

– Lamivudine: L180M +/- M204V/I (YMDD)– Adefovir: N236T and A181V– Entecavir: I169, T184, S202 and M250 (LAMR

patients)– Telbivudine: M204I

1Chu CJ, et al. Gastroenterology. 2003;125:444-451.2Keeffe EB, et al. Clin Gastroenterol Hepatol. 2006;4:936-962.

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● Epidemiology

● Hepatitis C Virus natural History

● HCV/HIV Co-infection

● Novel drug therapies

● HBV infection

● HBV vaccinations

Outline

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HBV Vaccination

● Of persons who did not respond to a primary 3-dose vaccine series with anti-HBs concentrations of >10 mIU/mL, 25%--50% responded to an additional vaccine dose, and 44%--100% responded to a 3-dose revaccination series.

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HBV Vaccination

● Better response to revaccination occurs in persons who have measurable but low (<10 mIU/mL) levels of antibody after the initial series

● Increased vaccine doses (e.g., double the standard dose) were demonstrated to enhance revaccination response rates in one study but not in another .

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Thank You

Dushyantha Jayaweera, M.D., M.R.C.O.G., F.A.C.P.

Professor in Clinical Medicine

Division of Infectious Diseases

University of Miami Miller School of Medicine