Hepatitis B virus: Difference between revisions
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* Reverse-transcription double-stranded DNA (RT-dsDNA) virus |
* Reverse-transcription double-stranded DNA (RT-dsDNA) virus |
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* Genotypes A through J vary in geographic distribution and clinical severity |
* Genotypes A through J vary in geographic distribution and clinical severity |
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{| class="wikitable" |
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! Genotype !! B !! C !! A !! D !! E-J |
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|- |
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! colspan=6 | Clinical characteristics |
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|- |
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| Modes of transmission |
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| Perinatal/vertical |
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| Perinatal/vertical |
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| Horizontal |
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| Horizontal |
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| Horizontal |
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|- |
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| Tendency of chronicity |
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| Lower |
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| Higher |
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| Higher |
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| Lower |
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| No data |
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|- |
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| HBeAg positivity |
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| Lower |
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| Higher |
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| Higher |
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| Lower |
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| No data |
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|- |
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| HBeAg seroconversion |
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| Earlier |
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| Later |
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| Earlier |
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| Later |
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| No data |
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|- |
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| HBsAg seroclearance |
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| More |
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| Less |
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| More |
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| Less |
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| No data |
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|- |
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| Histological activity |
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| Lower |
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| Higher |
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| Lower |
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| Higher |
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| No data |
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|- |
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! colspan=6 | Clinical outcomes |
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|- |
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| Response to interferon-α |
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| Higher |
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| Lower |
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| Higher |
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| Lower |
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| Lower in G |
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|- |
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| Response to NRTIs |
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| colspan=4 | No significant differences |
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| No data |
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|- |
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! colspan=6 | Viroloical characteristics |
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|- |
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| Viral load |
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| Lower |
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| Higher |
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| colspan=3 | No data |
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|- |
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| Frequency of PC A1896 mutation |
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| Higher |
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| Lower |
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| Lower |
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| Higher |
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| No data |
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|- |
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| Frequency of basal core promoter T1762/A1764 mutation |
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| Lower |
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| Higher |
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| Higher |
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| Lower |
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| No data |
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|- |
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| Frequency of preS deletion utation |
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| Lower |
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| Higher |
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| colspan=3 | No data |
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|} |
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== Clinical Presentation == |
== Clinical Presentation == |
Revision as of 13:30, 25 June 2020
Background
Microbiology
- Reverse-transcription double-stranded DNA (RT-dsDNA) virus
- Genotypes A through J vary in geographic distribution and clinical severity
Genotype | B | C | A | D | E-J |
---|---|---|---|---|---|
Clinical characteristics | |||||
Modes of transmission | Perinatal/vertical | Perinatal/vertical | Horizontal | Horizontal | Horizontal |
Tendency of chronicity | Lower | Higher | Higher | Lower | No data |
HBeAg positivity | Lower | Higher | Higher | Lower | No data |
HBeAg seroconversion | Earlier | Later | Earlier | Later | No data |
HBsAg seroclearance | More | Less | More | Less | No data |
Histological activity | Lower | Higher | Lower | Higher | No data |
Clinical outcomes | |||||
Response to interferon-α | Higher | Lower | Higher | Lower | Lower in G |
Response to NRTIs | No significant differences | No data | |||
Viroloical characteristics | |||||
Viral load | Lower | Higher | No data | ||
Frequency of PC A1896 mutation | Higher | Lower | Lower | Higher | No data |
Frequency of basal core promoter T1762/A1764 mutation | Lower | Higher | Higher | Lower | No data |
Frequency of preS deletion utation | Lower | Higher | No data |
Clinical Presentation
Acute
- 75% are asymptomatic
- Symptoms range from self-resolving jaundice to fulminant liver failure in about 5%
Chronic
Investigations
Management
Acute
- Supportive care
Chronic
- HBsAg present ≥6 months
- HBV-DNA is variable
- Can be HBeAg positive or negative, with generally higher HBV DNA levels in HBeAg-positive patients
- ALT can be normal or elevated
- Liver boipsy shows chronic hepatitis and variable necroinflammation or fibrosis
Immune-active
- HBsAg present ≥6 months and HBeAg either positive or negative
- Intermittently or persistently elevated ALT and AST
Indications for treatment
- ALT ≥2x ULN or evidence of significant histologic disease, AND
- Elevated HBV DNA
- > 2000 IU/mL if HBeAg negative
- > 20,000 IU/mL if HBeAg positive
Immune-tolerant
- HBsAg present for ≥6 months and HBeAg positive
- HBV DNA typically over 1 million
- Normal or minimally-elevated ALT and AST
- That is, high viral load but normal ALT
Indications for treatment
- Adults >40 years, AND
- ALT rises above 2x ULN (i.e. becomes immune-active), OR
- Liver biopsy showing significant necroinflammation or fibrosis
Surveillance
- Monitor at 3 to 6 month intervals, more frequently as ALT levels rise, consider treatment if >2x ULN/
Treatment Regimens
- One of pegylated-interferon (48 weeks), tenofovir (until 12 months post-HBeAg conversion), or entecavir (until 12 months post-HBeAg conversion)
- Peg-IFN contraindicated in autoimmune disorders, uncontrolled psychiatric disease, cyptopenia, severe cardiac disease, uncontrolled seizures, and decompensated cirrhosis
- Peg-IFN preferred in lamivudine resistance
- Tenofovir is safe in pregnancy
- Duration depends on what stage is being treated
- HBeAg positive and HBV DNA >20,000 and ALT >2 ULN
- Peg-IFN for 48 weeks
- Tenofovir or entecavir for at least 12 months after HBeAg seroconversion (Ag to Ab)
- HBeAg negative and HBV DNA > 2000 and ALT >2x ULN (or biopsy shows necroinflammation or fibrosis, or non-invasive testing shows fibrosis)
- Peg-IGN for 1 year
- Tenofovir or entecavir for many years, possibly indefinitely
- HBeAg positive and HBV DNA >20,000 and ALT >2 ULN
- Continue HCC surveillance regardless of treatment
Inactive chronic hepatitis B
- Defined by HBeAg-negative, anti-HBeAb-positive, normal ALT, and HBV DNA <2000 IU/mL
- Monitor ALT q3mo for 1 year, then q6-12mo
- If ALT rises, check HBV-DNA and HBsAg for activity
HCC screening
- Screen if HBsAg-positive with cirrhosis, or HBsAg-positive at higher risk (Asian men >40yrs, black men >40yrs, Asian women >50yrs, family history, HDV coinfection)
- First-line is ultrasound every 6 months
- Second-line is AFP levels every 6 months
Prophylaxis in Immunosuppression
- Concern especially with chronic steroids and rituximab
- Can have the following effects
- Asymptomatic HBV DNA and ALT
- Hepatic failure
- Death
- If ≥7.5mg/d should be screened
- HBsAg +/- HBcAb if they're adding a second agent (rituximab, TNF-alpha inhibitors, or other)
- Refer to Hepatology or Infectious Diseases
- Prophylaxis with lamivudine until 6 months after chemotherapy
Further Reading
- Update on prevention, diagnosis, and treatment of chronic hepatitis B: AASLD 2018 hepatitis B guidance
- Hepatitis B virus genotypes: Global distribution and clinical importance. World J Gastroenterol. 2014;20(18):5427–5434. doi: 10.3748/wjg.v20.i18.5427
References
- ^ Mustafa Sunbul. Hepatitis B virus genotypes: Global distribution and clinical importance. World Journal of Gastroenterology. 2014;20(18):5427. doi:10.3748/wjg.v20.i18.5427.
- ^ Carla S. Coffin, Scott K. Fung, Fernando Alvarez, Curtis L. Cooper, Karen E. Doucette, Claire Fournier, Erin Kelly, Hin Hin Ko, Mang M Ma, Steven R Martin, Carla Osiowy, Alnoor Ramji, Edward Tam, Jean Pierre Villeneuve. Management of Hepatitis B Virus Infection: 2018 Guidelines from the Canadian Association for the Study of Liver Disease and Association of Medical Microbiology and Infectious Disease Canada. Canadian Liver Journal. 2018;1(4):156-217. doi:10.3138/canlivj.2018-0008.