Tak Won Young, Yang Jin Mo, Kim Byung Ik, Baik Soon Koo, Cheon Gab Jin, Byun Kwan Soo, Kim Do Young, Yoo Byung Chul
Department of Internal Medicine, Kyungpook National University Hospital, Daegu, Republic of Korea.
Department of Internal Medicine, The Catholic University Medical College St. Vincent's Hospital, Suwon, Republic of Korea.
Hepatol Int. 2014 May 25;8(3):375-81. doi: 10.1007/s12072-014-9537-5. eCollection 2014 Jul.
Clevudine 30 mg showed potent antiviral activity with a marked post-treatment antiviral effect. However, long-term treatment with clevudine monotherapy induced resistance and myopathy in some cases. The objective of this study is to evaluate the preliminary efficacy and safety of the combination of clevudine 20 mg and adefovir compared to clevudine monotherapy.
Seventy-four patients were randomized to either a combination of clevudine 20 mg and adefovir or clevudine 20 or 30 mg and were treated for 2 years. The viral kinetics for 24 weeks, virological response [VR; hepatitis B virus (HBV) DNA less than 300 copies/ml], and the biochemical response [BR; normal alanine aminotransferase (ALT)] were assessed.
There was no difference in baseline characteristics among the three groups. Viral kinetics study showed no statistically significant difference among them during 24 weeks. The combination group showed 95 % virological response with a statistically significant difference compared to the clevudine 30 mg (67 %) and 20 mg (71 %) groups (p = 0.0376). Biochemical response rates were similar in all groups (78-94 %). No resistance was reported in the combination group, while 20 % of patients treated with clevudine 30 mg or 20 mg reported resistance during 2 years. Muscle-related symptoms such as myalgia (1 in clevudine 30 mg, 1 in the combination group) and muscle weakness (1 in clevudine 30 mg, 2 in clevudine 20 mg) were reported in five patients (7 %); of these, three patients discontinued the study.
We concluded that the combination of clevudine 20 mg and adefovir produced a potent antiviral response together with a good resistance profile compared to clevudine monotherapy at 96 weeks in this pilot study.
30毫克克来夫定显示出强效抗病毒活性,并具有显著的治疗后抗病毒效果。然而,克来夫定单药长期治疗在某些情况下会诱导耐药性和肌病。本研究的目的是评估20毫克克来夫定与阿德福韦联合用药相较于克来夫定单药治疗的初步疗效和安全性。
74例患者被随机分为接受20毫克克来夫定与阿德福韦联合治疗组,或20毫克或30毫克克来夫定单药治疗组,并接受为期2年的治疗。评估了24周的病毒动力学、病毒学应答[VR;乙型肝炎病毒(HBV)DNA低于300拷贝/毫升]和生化应答[BR;丙氨酸转氨酶(ALT)正常]。
三组患者的基线特征无差异。病毒动力学研究显示,在24周期间三组之间无统计学显著差异。联合治疗组的病毒学应答率为95%,与30毫克克来夫定组(67%)和20毫克克来夫定组(71%)相比有统计学显著差异(p = 0.0376)。所有组的生化应答率相似(78 - 94%)。联合治疗组未报告耐药情况,而接受30毫克或20毫克克来夫定治疗的患者中有20%在2年期间报告了耐药。5例患者(7%)报告了与肌肉相关的症状,如肌痛(30毫克克来夫定组1例,联合治疗组1例)和肌无力(30毫克克来夫定组1例,20毫克克来夫定组2例);其中3例患者停止了研究。
我们得出结论,在本初步研究中,与克来夫定单药治疗相比,20毫克克来夫定与阿德福韦联合用药在96周时产生了强效抗病毒应答,并具有良好的耐药情况。
