Viral Hepatitis
Prof. MUDr. Petr Husa, CSc.
Klinika infekčních chorob, FN Brno
j0115884

Viral Hepatitis
1.Enterically transmitted – no chronic stage
•VH A
•VH E – extremely rare (IS)
2.Parenterally transmitted – possible chronic stage
•VH B
•VH C
•VH D

Healthy liver
Healthy Liver small Drawn Liver


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Liver fibrosis
Fibrosis small Drawn Fibrosis


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Liver cirrhosis
Drawn Cirrhosis Cirrhosis


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varixy6



varixy5



cirhotik1



cirhotik2



cirhotik3



cirhotik4



cirhotik5



CIH-VHC-caput medusae



ascites1



ascites2



Hepatocellular carcinoma
small Drawn Cancer Carcinoma


2002
2003
2004
2005
2006
2007
2008
2009
2010
2011
VH A
127
114
70
322
132
128
1648
1104
862
264
VH B
413
370
392
361
307
307
306
247
244
192
VH C
858
846
868
844
1022
980
974
836
709
812
VH E
12
21
36
37
35
43
65
99
72
163
Viral Hepatitis in CR 2002-2011
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A
B
C
D
E
Genom
RNA
DNA
RNA
RNA
RNA
Incubation
15-50
30-180
15-180
30-180
15-60
Enteral
Yes
No
No
No
Yes
Parenteral
Rare
Yes
Yes
Yes
No
Sexual
Rare
Yes
Rare
Yes
Rare
Vertical
No
Yes
Rare
Yes
Yes
Chronicity
No
Yes
Yes
Yes
Very rare
Vaccination
Yes
Yes
No
VH B
No
Imunoglob.
Yes
Yes
No
VH B
No

hepatitis a virus
Hepatitis A
family Picornaviridae, genus Hepatovirus – non-enveloped RNA, 27 nm

Global_HepA_ITHRiskMap
Hepatitis A


Epidemiology
•Fecal –oral route of transmission
üContaminated hands or daily used instruments
üContaminated drinking water
üContaminated food
•
•Vaccination available, recommended especially fore travelers to countries with lower standard of
hygiene
dlane

Concentration of Hepatitis A Virus graph



hepatitis a virus infection graph



Hepatisi B Virus
 Hepatitis B
family Hepadnaviridae, enveloped DNA virus, 42 nm

Global significance of HEP B
•One of the biggest global health problems
üMore than 2 billions of infections during the life
ü350-400 million chronic carriers - China (125 million), Brazil (3,7 million), South Korea (2,6
million), Japan (1,7 million), USA (more than 1 million), Italy (900 thousand).
ü25-40 % chronic carriers have LC or HCC, 0,5-1,0 million death due to decompensated LC or HCC
ü50 thousand death annually due to fulminant hepatitis
üGlobal vaccination in 177 countries (2008)
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Hepatitis B



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Hepatitis B in Czech Republic
•Still important infection but incidence and prevalence are gradually decreasing
üPrevalence of chronic carriers was 0.56 % (2001)
üPrevalence of historical antibodies anti-HBc total was 5,59% (2001)
üDecrease of prevalence and incidence due to vaccination of high-risk persons (health care workers,
newborns of HBsAg-positive mothers, before hemodialysis)
üGlobal vaccination of all newborns and 12-years old children since  2001
•
•

Epidemiology of HEP B
•Transmission
ü blood and blood products
ü sexual intercourse
ü organ and tissue transplant recipients
ü vertically from mother to newborn
•Who is in the highest risk in well-developed countries?
ü intravenous drug abusers
ü persons with multiple sexual partners
•
HM00316_ playmate_01

Clinical pictures of acute HEP B
•IP: 30–180 days (mostly 2–3 months)
•Prodromal stage -  flu-like syndrome
•Icteric form: < 5 years < 10 %, >  5 years (30–50 %)
•Chronicity: newborns > 90 %, children 30-40 %, adults 5–10 %
•Fulminant hepatitis: < 1 %
•Chronic HBV infection mortality: 15 – 25 %
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Outcome of Hepatitis B Virus Infection by Age at Infection (graph)



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c_virus
Hepatitis C
family Flaviviridae, genus Hepacivirus, enveloped RNA virus 60 nm

•
Hepatitis C
World Health Organization. Wkly Epid Rec .1999;74:425-427. World Health Organization. Hepatitis C:
Global Prevalence: Update. 2003. Farci P, et al. Semin Liver Dis. 2000;20:103-126. Wasley A, et al.
Semin Liver Dis. 2000;20:1-16.
Europe
8.9 million
(1.03%)
Americas
13.1 million
(1.7%)
Africa
31.9 million
(5.3%)
Western Pacific
62.2 million
(3.9%)
Eastern Mediterranean
21.3 million
(4.6%)
Southeast Asia
32.3 million
(2.15%)

HCV, hepatitis C virus.
The World Health Organization has estimated that approximately 170 million persons are infected
with HCV worldwide. The distribution of HCV infection is not uniform around the world. In most
places, approximately 1% to 2% of the population is infected with HCV, but some regions, such as
Egypt, are burdened with rates that range from 10% to 20%. HCV screening is the first step in
identifying the 170 million HCV-infected persons worldwide.

Distribution of HCV genotypes



Hepatitis C
•Significant global health problem
üabout 3 % of the world population are chronically infected with HCV
üIn well-developed countries about 20 % of all acute hepatitis, 70 %  chronic hepatitis, 40 %
cirrhosis, 60 % HCC and indication to 30 %  liver transplantations
•In Czech Republic
üprevalence 0,2 %  (2001)
•No vaccine, no hyper-immune immunoglobulin
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Epidemiology of HEP C
•Transmission:
ü blood and blood products
ü sharing of used injection needles and syringes
ü sexually (rare)
ü vertically (rare)
•Who is in the highest risk of HCV infection at present?
ü intravenous drug abusers
•Infection is frequently diagnosed in chronic stage
•
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Patients with higher risk of HCV infection
PIntravenous drug abusers (sharing of injection needles and syringes)
PRecipients of blood transfusions before the year 1992 (especially hemophiliacs)
PPersons with tattoo or piercing

Clinical course of HEP C
•Acute hepatitis is mostly asymptomatic
•Probability of chronicity is high (40-50% till 90-100%).
•Higher probability of chronicity:
aOlder persons
aHigher initial infection dose (transfusion versus needles)
aHBV, HIV co-infection
aabusus of alcohol
aimmunodeficiency

Clinical course of HEP C
•LC in about 20 % patients with chronic HCV infection
•HCC annually in 1-4 % patients with LC
•Progression to HCC depends on:
üage (more rapid progression in older persons)
üalcohol abuse
üHIV co-infection
üHBV co-infection
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Serologic Pattern of Acute HCV Infection w/ Recovery



Serologic Pattern of Acute HCV Infection w/ Progression to Chronic Infection



Hepatitis D (Delta) Virus (photo and diagram)
Hepatitis D
Satelite virus, family Deltaviridae, enveloped RNA, 40 nm

Hepatitis D
•Ability of replication only in presence of HBV infection
üCo-infection (better prognosis)
üSuper-infection (worse prognosis)
•Endemic in South America, Mediterranean Region, Romania, Central Africa
•Very low prevalence in CR
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Anti-HDV prevalence in HBsAg-positive
(approximately 15 000 000 persons)
Rizzetto M. EASL 2009

•
Drug addicts
Rizzetto M. EASL 2009

Diapositiva1
2010s
:
• immigrants
2009
Rizzetto M. EASL 2009

koinfekce



superinfekce



Hepatitis E Virus (photo)
Family Hepeviridae, genus Hepevirus, non-enveloped RNA virus, 27-34 nm


hepatitida E
Hepatitis E
Source: CDC

HEV0002
HEV genotypes
Purcell RH, Emerson SU. J Hepatol 48 (2008) 494-503

HEV0003
Genotypes of swine HEV
Purcell RH, Emerson SU. J Hepatol 48 (2008) 494-503

Hepatitis E
•Travel-related disease especially
•Infection is possible to acquire in CR as well (pork, sea food)
•Main route of transmission by drinking water
•Extremely serious clinical course in late pregnancy (mortality above 20 %)
•Repeated infection may be possible
•Rare cases of chronic hepatitis E in seriously immunosuppressed patients (organ recipients…)
•
•
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HEV Serology (graph)



Treatment of acute hepatitis
•Symptomatic for all types
ü physical and mental rest
ü diet
ü no alcohol, no hepatoxic drugs
ü supportive treatment (silymarin, essential phosholipids)
•
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Current possibilities of treatment of chronic HBV infection
•pegylated interferon alfa-2a – 48 weeks
•lamivudine  - only in severe acute HEP B or protection of reactivation or recurence
•telbivudine – for naive patients
•entecavir – for naive patients
•adefovir dipivoxil – for lamivudine-resistant mutants in combination with lamivudine
•tenofovir – both for naive and lamivudine-resistant patients
•

Resistance to NUCs



Current possibilities of treatment of chronic HCV infection
•Pegylated interferon alfa-2a or alfa-2b + ribavirin
üGenotype 1 or 4 – 48 weeks, SVR about 60 %
üGenotype 2 or 3 – 24 weeks, SVR about 85 %

Standard chronic hepatitis C therapy
•genotypes 1,4
üPEG-IFN + RBV (1000-1200mg) - 48 weeks
üPEG-IFN + RBV + DAA (boceprevir or telaprevir) – response guided therapy – 24-48 weeks
•genotypes 2-3
üPEG-IFN+RBV (800 mg) – 24 weeks

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HCV Life Cycle and DAA Targets
Adapted from Manns MP, et al. Nat Rev Drug Discov. 2007;6:991-1000.
Receptor binding
and endocytosis
Fusion and
uncoating
Transport
and release
(+) RNA
Translation and
polyprotein processing
RNA replication
Virion
assembly
Membranous
web
ER lumen
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LD
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LD
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ER lumen
LD
•
NS3/4 protease inhibitors
NS5B polymerase inhibitors
Nucleoside/nucleotide
Nonnucleoside
*Role in HCV life cycle not well defined
NS5A* inhibitors

DAAs, direct-acting antivirals; ER, endoplasmic reticulum; HCV, hepatitis C virus; LD, luminal
domain.
The elucidation of the life cycle of the hepatitis C virus (HCV) allowed for the identification of
potential targets of antivirals that directly interrupt HCV replication. From the binding of the
virus to the plasma membrane and its endocytosis through the membrane, all the way through
uncoating and generating the membranous web to translation and replication, viral assembly, and
transport and release again into the extracellular space, one may envision a variety of potential
targets. The most obvious targets are the NS3/4 serine protease and the NS5B HCV polymerase.
Therefore, our first DAAs have been protease inhibitors and nucleoside or nonnucleoside polymerase
inhibitors.
Also interesting was the recent discovery of NS5A inhibitors that are inhibitors of the NS5A
protein. However, the function of this protein in the hepatitis C life cycle is not yet well
understood. Therefore, the inhibitory drugs may help to elucidate the involvement of this protein
in the HCV life cycle rather than vice versa.

Efficacy of chronic hepatitis C therapy
0
20
40
60
80
100
naive
experienced
38-44[1-2]
17-21[3-4]
PEG IFN/RBV
0
20
40
60
80
100
63-75[1-2]
59-66[3-4]
PEG IFN/RBV+TVR, BOC
1. Poordad F, et al. AASLD 2010. Abstract LB-4. 2. Jacobson IM, et al. AASLD 2010. Abstract 211. 3.
Bacon BR, et al. AASLD 2010. Abstract 216. 4. Foster GR, et al. APASL 2011. Abstract 1529.
naive
experienced

BOC, boceprevir; GT1, genotype 1; SOC, standard of care; SVR, sustained virologic response; TPV,
telaprevir.
This slide is a summary of data. It is clearly not a head-to-head comparison but an illustration of
the data for boceprevir and telaprevir in patients who were treatment naive or previous
nonresponders. If one compares the blue box on the left with the blue box on the right, one can see
that in treatment-naive patients, approximately 30% more patients can be cured with the addition of
either boceprevir or telaprevir to peginterferon/ribavirin. The difference is even more pronounced
in previous nonresponders. Here one can see success rates of 17% to 21% with repeat
peginterferon/ribavirin treatment; however, a 59% to 66% SVR rate can be attained in these previous
nonresponders when a protease inhibitor is added. So you clearly see how important, especially for
patients who have been previously unsuccessfully treated, the addition of a protease inhibitor will
be.

husa-tenisky Thank you for your attention! phusa@fnbrno.cz