Hepatitis B medical therapy
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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Chetan Lokhande, M.B.B.S [2]
Medical Therapy
Goal of therapy
- Eradicate the virus from the body
- Prevent progression of end stage liver disease (ESLD)
- Prevent progression to hepatocellular carcinoma (HCC)
- Clear off HBV DNA
- HBeAg and HBsAg negative
- Normal ALT / AST
- Normal histology
Indications to start antiviral medications
- Following are the curent indications to start treatment for chronic hepatits B:[1]
- Chronic hepatitis B ( HbeAg postive and negative ) with HBV DNA >2000 IU/ml and/or
- Elevated ALT and
- Severe necrosis and fibrosis on biopsy
- Decompensated or compensated cirrhosis with normal ALT or HBV DNA <2000 IU/ml
- Treatment should be continued for atleast 6 months after HBeAg loss / conversion.
Antiviral Medications
There are three types of treatment groups:
- IFN
- Nucleoside analogs
- Nucleotide analogs
First Line agents
Entecavir (ETV)
- An anti-HBV nucleoside analog
- A 94% clearance rate after 5 years of treatment is observed in HBeAg positive patients.[2]
- A 90% clearance rate after 48 weeks of treatment is observed in HBeAg negative patients.[3]
- A necroinflammation improvement of 96% and fibrosis improvement of 88% is seen after a treatment for 6 years.[2]
Tenofovir (TDF)
- An anti-HBV nucleotide analog
- A 68% clearance rate in HBV DNA after 4 years of treatment is observed in HBeAg positive patients.[4]
- A 84% clearance rate in HBV DNA after 4 years of treatment is observed in HBeAg negative patients.
Interferons
- Antiviral and antiproliferative glycoprotein.
- No antiviral resistance have been noted
- Best results noted with genotype A or B who are HBeAg positive.
Second line agents
Telbivudine (LDT)
- Nucleoside analog
- Worse resistance than first line agents and not indicated if resistance to other nucleoside analogs are noted.
Adefovir (ADV)
- Nucleotide analog
- Worse resistance than first line agents
- Used in cases of nucleotide analog resistance.
Lamivudine
- Nucleoside analog
- Has a high rate of resistance and hence not used currently.
Medical Therapy
In the first few months of infection, hepatitis B does not usually get treated. Up to 95% of adults clear the infection spontaneously without treatment. Therapy in this stage of infection does not seem to further improve the chances of spontaneous cure. Early antiviral treatment may only be required in fewer than 1% of patients, whose hepatitis B takes a very aggressive course ("fulminant hepatitis").
There are currently several treatments for chronic hepatitis B. While none of the available drugs usually clear the infection, they can stop the virus from replicating, and prevent liver damage such as cirrhosis and/or liver cancer. Treatments are available in the form of antiviral drugs such as lamivudine, adefovir, entecavir or telbivudine, and immune system modulators such as interferon alpha (Uniferon) or peg-interferon alpha (PEGASYS). There are several other antivirals under investigation. However, some individuals are much more likely to respond than others. It does not appear that combination therapy offers any advantages,[5] but may help in patients with resistant viruses, or in advanced liver disease where resistant viruses may lead to liver failure. In general, each treatment works by reducing the viral load by several orders of magnitude. In some patients, chronic hepatitis B takes a mild course and does not require immediate treatment. Treatment strategies should be individualized. Considerations include a person's risk for developing complications of persistent infection, a person's likelihood of adhering and responding to treatment, and potential risks such as side effects or development of viral resistance.
On March 29, 2005, the US Food and Drug Administration (FDA) approved Entecavir for the treatment of hepatitis B.[6]
On February 25, 2005, the EU Commission approved PEGASYS for the treatment of hepatitis B making it the first pegylated interferon to be approved for hepatitis B.[7]
On October 27, 2006, telbivudine gained FDA approval for treatment of chronic hepatitis B. It is marketed under the brand name Tyzeka in the US and Sebivo outside the US. It is already approved in Switzerland.[8]
Chronic carriers are encouraged to avoid consuming alcohol as it increases their risk for cirrhosis and hepatocellular carcinoma (liver cancer).
Infants born to mothers known to carry hepatitis B can be treated with antibodies to the hepatitis B virus (hepatitis B immune globulin or HBIg). When given with the vaccine within twelve hours of birth, the risk of acquiring hepatitis B is reduced 95%. This treatment also allows a mother to safely breastfeed her child.
An individual exposed to the virus who has never been vaccinated may be treated with HBIg immediately following the exposure. For instance, a health care worker accidentally stuck by a needle used in a hepatitis B carrier would qualify. Treatment must be soon after exposure, however.
As a summary:
There are no medications available for recently acquired (acute) HBV infection. Hepatitis B vaccine is available for the prevention of HBV infection. There are antiviral drugs available for the treatment of chronic HBV infection.
- HBV infected persons should be evaluated by their doctor for liver disease.
- Adefovir dipivoxil, interferon alfa-2b, pegylated interferon alfa-2a, lamivudine, entecavir, and telbivudine are six drugs used for the treatment of persons with chronic hepatitis B.
- These drugs should not be used by pregnant women.
- Drinking alcohol can make liver disease worse.
Recommendations on Whom to Treat and with What Antiviral Agent: AASLD Practice Guidelines 2009[9]
“ |
1. Patients with HBeAg-positive chronic hepatitis B
2. Patients with HBeAg-negative chronic hepatitis B (serum HBV DNA >20,000 IU/mL and elevated ALT >2 times normal) should be considered for treatment. (Grade I)
3. Patients who failed to respond to prior IFN-α (standard or pegylated) therapy may be retreated with nucleoside analogues (NA) if they fulfill the criteria listed above. (Grade I) 4. Patients who failed to achieve primary response as evidenced by <2 log decrease in serum HBV DNA level after at least 6 months of NA therapy should be switched to an alternative treatment or receive additional treatment. (Grade III) 5. Patients who develop breakthrough infection while receiving NA therapy
6. Treatment of patients with lamivudine (or telbivudine)-resistant HBV
should be stopped as continued presence of lamivudine- (or telbivudine-) resistant mutations will increase the risk of entecavir resistance. (Grade II-3 for lamivudine-resistant HBV and Grade III for telbivudine-resistant HBV). Entecavir is not an optimal therapy because of increasing risk of resistance to entecavir over time. (Grade II-2) 7. Treatment of patients with adefovir-resistant HBV
8. Treatment of patients with entecavir-resistant HBV
9. Patients with compensated cirrhosis — Treatment should be considered for patients with ALT >2 times normal, and for patients with normal or minimally elevated ALT if serum HBV DNA levels are high (>2,000 IU/mL). (Grade II-2)
10. Patients with decompensated cirrhosis — Treatment should be promptly initiated with a NA that can produce rapid viral suppression with low risk of drug resistance. (Grade II-1)
11. In patients with inactive HBsAg carrier state antiviral treatment is not indicated, but these patients should be monitored. |
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Recommendations for Dose Regimens: AASLD Practice Guidelines 2009[9]
“ |
1. IFN-α and pegIFN-α are administered as subcutaneous injections.
2. Lamivudine is administered orally.
3. Adefovir is administered orally.
4. Entecavir is administered orally.
5. Telbivudine is administered orally.
6. Tenofovir is administered orally.
7. Duration of nucleoside analogue treatment
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Recommendations for Initial Evaluation of Persons with Chronic HBV Infection: AASLD Practice Guidelines 2009[9]
“ |
1. Initial evaluation of persons newly diagnosed with chronic HBV infection should include history, physical examination and laboratory testing. (Grade III) 2. All persons with chronic hepatitis B not immune to hepatitis A should receive 2 doses of hepatitis A vaccine 6 to 18 months apart. (Grade II-3) |
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Recommendations for Treatment of Patients with Acute Symptomatic Hepatitis B: AASLD Practice Guidelines 2009[9]
“ |
1. Treatment is only indicated for patients with fulminant hepatitis B and those with protracted, severe acute hepatitis B. (Grade III) 2. Lamivudine or telbivudine may be used when the anticipated duration of treatment is short; otherwise, entecavir is preferred. (Grade II-3)
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References
- ↑ "http://www.easl.eu/assets/application/files/ef520780b91cf4f_file.pdf" (PDF). External link in
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(help) - ↑ 2.0 2.1 "Chronic Hepatitis B: Integrating Long-Term Treatment Data and Strategies to Improve Outcomes in Clinical Practice".
- ↑ Lai, CL.; Shouval, D.; Lok, AS.; Chang, TT.; Cheinquer, H.; Goodman, Z.; DeHertogh, D.; Wilber, R.; Zink, RC. (2006). "Entecavir versus lamivudine for patients with HBeAg-negative chronic hepatitis B.". N Engl J Med. 354 (10): 1011–20. doi:10.1056/NEJMoa051287. PMID 16525138. Unknown parameter
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ignored (help) - ↑ "http://jid.oxfordjournals.org/content/204/3/415.full". External link in
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(help) - ↑ Lau GKK; et al. (2005). "Peginterferon Alfa-2a, lamivudine, and the combination for HBeAg-positive chronic hepatitis B". N Engl J Med. 352 (26): 2682–95. PMID 15987917.
- ↑ U.S. Food and Drug Administration. March 30, 2005. FDA Talk Paper: FDA Approves New Treatment for Chronic Hepatitis B. fda.gov. Retrieved on September 11, 2007.
- ↑ February 25, 2005. Pegasys approved in the European Union for the treatment of chronic hepatitis B: Only pegylated interferon approved for the treatment of chronic hepatitis B. roche.com. Retrieved on September 11, 2007.
- ↑ October 27, 2006. FDA Approves Telbivudine for Treatment of Chronic Hepatitis B. hivandhepatitis.com. Retrieved on September 11, 2007.
- ↑ 9.0 9.1 9.2 9.3 Lok AS, McMahon BJ (2004). "[AASLD Practice Guidelines. Chronic hepatitis B: update of therapeutic guidelines]" (PDF). Romanian Journal of Gastroenterology. 13 (2): 150–4. PMID 15229781. Retrieved 2012-02-10. Unknown parameter
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ignored (help)