Shim Ju Hyun, Suh Dong Jin, Kim Kang Mo, Lim Young-Suk, Lee Han Chu, Chung Young-Hwa, Lee Yung Sang
Department of Internal Medicine, Asan Medical Center, University of Ulsan College of Medicine, Seoul, Korea.
Hepatology. 2009 Oct;50(4):1064-71. doi: 10.1002/hep.23145.
Entecavir (ETV) is currently recommended as a rescue therapy purely for adefovir (ADV)-resistant chronic hepatitis B virus (HBV) infections. We evaluated the efficacy of ETV in patients who were resistant to lamivudine (LAM)/ADV sequential therapy and in those resistant to LAM monotherapy. Fifty LAM/ADV-resistant and 38 LAM-resistant patients who received ETV 1 mg/day for at least 48 weeks were enrolled. Mean baseline serum HBV DNA and alanine aminotransferase (ALT) levels were significantly lower in the LAM/ADV-resistant group, compared with the LAM-resistant group (6.90 versus 7.62 log(10) copies/mL and 102.6 versus 160.2 IU/L; both P < 0.05); hepatitis B e antigen (HBeAg) status and LAM-resistant mutation patterns were similar in the two groups. At week 48, mean reductions in HBV DNA and ALT levels were significantly less in the LAM/ADV-resistant group (-2.96 versus -4.86 log(10) copies/mL and -68.3 versus -128.9 IU/L; both P < 0.05). Achievement of undetectable HBV DNA was also less common in the LAM/ADV-resistant group (10.0% versus 34.2%; P = 0.006), although the rates of HBeAg loss and ALT normalization did not differ between the two groups. Resistance to both LAM and ADV was an independent risk factor for failure of HBV DNA negativity at week 48 (odds ratio, 0.138; P = 0.019). In both LAM/ADV-resistant and LAM-resistant groups, primary responders (> or =1 log decline in HBV DNA at week 12) achieved a significantly greater decrease in HBV DNA levels over the 48-week period, compared with primary nonresponders (-4.18 versus -0.97 and -5.37 versus -2.15 log(10) copies/mL, respectively; both P < 0.05).
The 48-week ETV treatment was less effective in LAM/ADV-resistant than in LAM-resistant patients. Continuing ETV monotherapy could be determined based on the virological response at 12 weeks in LAM/ADV-resistant patients.
目前恩替卡韦(ETV)仅被推荐作为对阿德福韦(ADV)耐药的慢性乙型肝炎病毒(HBV)感染的挽救治疗药物。我们评估了ETV对拉米夫定(LAM)/ADV序贯治疗耐药患者以及对LAM单药治疗耐药患者的疗效。纳入了50例对LAM/ADV耐药和38例对LAM耐药且接受每日1mg ETV治疗至少48周的患者。与LAM耐药组相比,LAM/ADV耐药组的平均基线血清HBV DNA和丙氨酸氨基转移酶(ALT)水平显著更低(分别为6.90对7.62 log₁₀拷贝/mL和102.6对160.2 IU/L;P均<0.05);两组的乙肝e抗原(HBeAg)状态和LAM耐药突变模式相似。在第48周时,LAM/ADV耐药组的HBV DNA和ALT水平的平均降低幅度显著更小(分别为-2.96对-4.86 log₁₀拷贝/mL和-68.3对-128.9 IU/L;P均<0.05)。在LAM/ADV耐药组中,实现HBV DNA检测不到的情况也较少见(10.0%对34.2%;P = 0.006),尽管两组的HBeAg消失率和ALT复常率没有差异。对LAM和ADV均耐药是第48周时HBV DNA未转阴的独立危险因素(比值比,0.138;P = 0.019)。在LAM/ADV耐药组和LAM耐药组中,与初始无应答者相比,初始应答者(第12周时HBV DNA下降≥1 log)在48周期间的HBV DNA水平下降幅度显著更大(分别为-4.18对-0.97和-5.37对-2.15 log₁₀拷贝/mL;P均<0.05)。
ETV治疗48周对LAM/ADV耐药患者的疗效低于对LAM耐药患者。对于LAM/ADV耐药患者,可根据12周时的病毒学应答情况来决定是否继续ETV单药治疗。
