Table 1.
Overview of epidemiology, symptoms, natural history and clinical management of viral hepatitis infections
|
Virus
|
Estimated number of infections worldwide
|
Mode of transmission
|
Typical clinical signs/symptoms
|
Natural history
|
Diagnosis
|
Treatment
|
Prevention
|
| Hepatitis A | 1.4 million annually | Fecal-oral route | Many asymptomatic. Most with non-specific symptoms of fatigue, nausea, vomiting, anorexia, jaundice | Asymptomatic, self-limited illness, prolonged cholestasis, relapsing, fulminant hepatitis (very rare) | Hepatitis A IgM | Supportive care, post-exposure vaccination and HAV immunoglobulin | Sanitation efforts, vaccination |
| Hepatitis B | 257million chronic HBV infections (WHO 2017 Global Hepatitis Report) | Vertical transmission (common for chonic HBV); IVDU, blood product transfusions, sexual contact (common for acute HBV) | Acute: non-specific symptoms (fatigue, nausea, vomiting, anorexia, jaundice); chronic: often asymptomatic, can progress to cirrhosis and HCC | Infection at birth: chronic HBV infection (immune tolerance, immune clearance, inactive carrier, reactivation). Eventual progression to cirrhosis and HCC; infection in adulthood: > 95% clearance | Past infection-HBsAg negative, HBsAb positive, HBcAb positive, HBeAb +/-; current infection-HBsAg positive, HBsAb negative, HBcAb positive, HBeAb +/- | Nucleot(s)ide reverse transcriptase inhibitors (entecavir, tenofovir); interferon | HBV vaccine (universal vaccination recommended at birth); HBIG in select cases |
| Hepatitis C | 71 million (WHO 2017 Global Hepatitis Report) | Direct blood stream inoculation (IVDU, unregulated tattoos/piercings, blood transfusion and organ transplants) | Typically asymptomatic until cirrhosis develops | Spontaneous clearance: 10%-25%; chronic Infection: 75%-90%, can progress to cirrhosis and HCC | HCV antibody, HCV RNA viral load | Direct acting antivirals | Widespread screening efforts |
| Hepatitis D | 12 million cases annually, 4.5% of HBV-infected individuals | Similar to Hepatitis B (IVDU, blood product transfusions, sexual contact) | Non-specific symptoms of fatigue, nausea, vomiting, anorexia, jaundice | Simultaneous coinfection of HDV and HBV: rare fulminant hepatitis, usually complete recovery; superinfection on chronic HBV: accellerated progression of chronic HBV | HDV IgM (acute), HDV IgG (chronic) | Hepatitis B treatment | Hepatitis B vaccination |
| Hepatitis E | 20 million acute infections (The Global Burden of Hepatitis E Virus Genotypes 1 and 2 in 2005) | Genotypes 1 and 2: Fecal-oral route; genotypes 3 and 4: Zoonotic, contaminated meat | Commonly asymptomatic; prodromal flu-like symptoms, nausea, vomiting, anorexia, fatigue followed by jaundice | Acute self-limited in majority of cases, severe in pregnant women; chronic hepatitis in immunocompromised hosts | HEV IgM (acute), HEV IgG (chronic) | Chronic infection: decrease immunosuppression, ribavirin | Genotypes 1 and 2: Sanitation efforts, vaccine available in China |
| Hepatitis G | 4.8% worldwide | Direct blood stream inoculation (IVDU, unregulated tattoos/piercings, blood transfusion and organ transplants) | Not well-described, likely asymptomatic | Not well-described. Unlikely to cause clinically significant hepatitis in humans. | Hepatitis G RNA; not currently used clinically | None | None |
HAV: Hepatitis A virus; HBV: Hepatitis B virus; HCV: Hepatitis C virus; HDV: Hepatitis D virus; HEV: Hepatitis E virus; HGV: Hepatitis G virus; WHO: World Health Organization; IVDU: Intravenous drug use; HCC: Hepatocellular carcinoma; HBIG Hepatitis B immunoglobulin; HBsAb: Hepatitis B surface antibody; HBsAg: Hepatitis B surface antigen; IgG: Immunoglobulin G; IgM: Immunoglobulin M.