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©2012 Baishideng.
World J Virol. Jun 12, 2012; 1(3): 71-78
Published online Jun 12, 2012. doi: 10.5501/wjv.v1.i3.71
Published online Jun 12, 2012. doi: 10.5501/wjv.v1.i3.71
HBV polymerase mutation(s) | Corresponding HBsAg mutation(s) | Clinical relevance | Effect(s) on HDV |
rtM204V | sI195M(A) | LMV resistance | Enhanced HDV secretion |
rtM204I | sW196L/S/stop | LMV resistance | S, L: no HDV secretion |
rtD205H | sW196F | Selected during LMV treatment with reduced binding to anti-HBsAg antibodies | Reduced HDV secretion |
rtV173L | sE164D | Selected during LMV treatment with reduced binding to anti-HBsAg antibodies | Reduced HDV secretion |
rtV173L/rtM204V | sE164D/sI195M | Selected during LMV treatment with reduced binding to anti-HBsAg antibodies | Support HDV secretion |
Ref. | Drug used | Dosage | No. of patients included | Main result (s) |
Garripoli et al[45], 1994 | Ribavirin monotherapy | 15 mg/kg for 16 wk | 9 | Ribavirin did not show significant antiviral effects in chronic hepatitis D |
Wolters et al[49], 2000 | LAM + IFN add-on | LAM 100 mg at least for 24 wk; afterwards combination therapy with IFN 9 MU/d for 4 wk, followed by 9 MU 3 times/wk for 12 wk | 8 | Neither LAM alone nor the addition of IFN was capable of reducing HDV |
Yurdaydin et al[47], 2002 | Famciclovir | 500 mg for 6 mo | 15 | Not effective |
Farci et al[40], 2004 | High-dose IFN αvs low dose IFN vs no treatment | High dose: 9 million units 3 times/wk, low dose 3 million units 3 times/wk for 48 wk | 36 | High-dose IFN α significantly improves long term clinical outcome and survival |
Kaymakoglu et al[46], 2005 | IFN α + ribavirin | IFN 10 MU 3 times/wk, Ribavirin 1000-1200 mg/d for 24 mo | 19 | Addition of Ribavirin to IFN-α does not increase response rate in patients with CHD |
Niro et al[36], 2005 | LAM vs placebo | 100 mg LAM for 52 wk | 31 | HDV viraemia was unaffected, even in patients when HBV replication was lowered by LAM therapy |
Erhardt et al[43], 2006 | PEG-IFN | 1.5 μg/kg PEG-IFN per wk for 48 wk | 12 | PEG-IFN is a promising treatment option in chronic hepatitis D |
Castelnau et al[41], 2006 | PEG-IFN | 1.5 μg/kg PEG-IFN per wk for 12 mo | 14 | PEG-IFN is safe and efficient for HDV treatment |
Niro et al[42], 2006 | PEG-IFN mono vs combination therapy with ribavirin | 1.5 μg/kg PEG-IFN per wk; 800 mg ribavirin; 48 wk mono or combination therapy, afterwards 24 wk PEG-IFN mono | 38 | Ribavirin had no effect |
Yurdaydin et al[50], 2008 | LAM vs LAM + IFN vs IFN mono | IFN 9MU 3 times/wk, LAM 100 mg; totally 12 mo therapy; for combination therapy 2 mo LAM mono, afterwards 10 mo combination | 39 | Addition of LAM to IFN is of no additional value; both (IFN mono/IFN + LAM) are superior to LAM mono |
Mansour et al[52], 2010 | PEG-IFN, add-on tenofovir und emtricitabine after 2 mo | PEG-IFN 180 μg/wk; tenofovir 300 mg/d for 10 mo | 1 | Combination therapy with PEG-IFN and nucleoside/tide analogue seems to be more effective than IFN alone |
Wedemeyer et al[44], 2011 | PEG-IFN mono vs adefovir vs combination PEG-IFN + adefovir | PEG-IFN 180 μg/wk; adefovir 10 mg/d for 48 wk | 90 | PEG-IFN α-2a with or without adefovir resulted in sustained HDV clearance in about 25% |
- Citation: Dastgerdi ES, Herbers U, Tacke F. Molecular and clinical aspects of hepatitis D virus infections. World J Virol 2012; 1(3): 71-78
- URL: https://www.wjgnet.com/2220-3249/full/v1/i3/71.htm
- DOI: https://dx.doi.org/10.5501/wjv.v1.i3.71