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恩替卡韦或其联合阿德福韦酯补救治疗拉米夫定联合阿德福韦酯应答不佳的慢性乙型肝炎
作者姓名:Xing J  Han T  Liu L  Li Y  Li J  Li Y  Xiao SX
作者单位:1. 300170天津医科大学三中心临床学院
2. 天津市第三中心医院肝病消化科;天津市肝胆疾病研究所;天津市人工细胞重点实验室
3. 天津市第三中心医院肝病消化科
基金项目:国家重点基础研究发展计划(973计划,国家“十一五”科技重大专项,天津市卫生局重点攻关资助项目
摘    要:目的 对拉米夫定(LAM)初治耐药后,LAM联合阿德福韦酯(ADV)应答不佳的慢性乙型肝炎患者,分别采用恩替卡韦(ETV)单药或ETV联合ADV进行补救治疗,比较两种补救方案的疗效.方法 对LAM初治耐药后应用LAM联合ADV应答不佳的40例患者,分别应用ETV 1.0 mg/d(14例)及ETV 0.5 mg/d联合ADV 10mg/d (26例)两种方案进行补救治疗,至少观察48周,定期监测HBV DNA、肝肾功能、HBV标志物等指标.根据资料不同分别采用t检验Wilcoxon检验或x2检验.结果 两组患者采用补救治疗前的基线情况差异无统计学意义.分别采用两种补救方案治疗后,两组患者HBV DNA水平均有下降,但ETV联合ADV组下降幅度较大.补救治疗24周时,ETV 1,0mg组有28.6%%(4例)达到HBV DNA转阴,ETV联合ADV组则有80.8% (21例)达到HBV DNA转阴,x2=8.469,P=0.004,差异具有统计学意义;48周时,ETV1.0mg组仍仅有4例患者HBV DNA转阴,而ETV联合ADV组全部26例患者均达到HBV DNA转阴.补救治疗24周时,ETV 1.0mg组有42.9%(6例)患者ALT复常,ETV联合ADV组有92.3% (24例)患者ALT复常,x 2=9.337,P=0.002,差异具有统计学意义;48周时,ETV 1.0mg组有57.1%(8例)患者ALT复常,而ETV联合ADV组所有患者均达到ALT复常.补救治疗48周时,ETV 1.0mg组有1例患者发生HBeAg血清学转换,ETV联合ADV组有4例患者发生HBeAg血清学转换.结论 对于LAM耐药后LAM联合ADV应答不佳的慢性乙型肝炎患者,采用ETV联合ADV的补救方案较ETV单药1.0mg的方案更为有效,可以实现更好的病毒学及生物化学应答.

关 键 词:肝炎  乙型  慢性  拉米夫定  阿德福韦酯  恩替卡韦

Entecavir 1.0mg monotherapy or entecavir plus adefovir dipivoxil for patients with lamivudine-resistant chronic hepatitis B had suboptimal response to lamivudine plus adefovir dipivoxil
Xing J,Han T,Liu L,Li Y,Li J,Li Y,Xiao SX.Entecavir 1.0mg monotherapy or entecavir plus adefovir dipivoxil for patients with lamivudine-resistant chronic hepatitis B had suboptimal response to lamivudine plus adefovir dipivoxil[J].Chinese Journal of Hepatology,2011,19(11):828-832.
Authors:Xing Jing  Han Tao  Liu Lei  Li Ying  Li Jun  Li Yan  Xiao Shi-xiang
Institution:Department of Hepatology, Third Central Hospital of Tianjin Medical University, Tianjin Key Laboratory of Artificial Cells, Tianjin 300170, China.
Abstract:Objective To evaluate the efficacy of entecavir (ETV) 1.0 mg/d or ETV plus adefovir dipivoxil (ADV) in adults with chronic hepatitis B virus (HBV) infection who had previously resisted lamivudine (LAM) and failed with rescue treatment of LAMd + ADV.Methods 40 patients were enrolled.14 patients were treated with ETV 1.0 mg/d monotherapy while 26 patients were treated with ETV 1.0 mg/d +ADV 10 mg/d.The HBV DNA level,liver function,HBV serology and renal function were observed.Results There was no statistically significant difference with baseline situation between group ETV 1.0 mg and group ETV + ADV.HBV DNA level in group ETV 1.0 mg was (5.768 ± 0.709) log10 copies/ml on baseline,and it declined to (4.712 ± 0.846) log10 copies/ml,(3.914 ± 0.996) log10 copies/ml,(3.702 ± 0.934) log10 copies/nil,(3.879 ± 0.913) log10 copies/ml and (3.855 ± 1.070) log10 copies/ml at 4,8,12,24 and 48 weeks.HBV DNA level in group ETV + ADV was (5.703 ± 0.845) log10 copies/ml on baseline,and it declined to (4.476 ± 0.905) log10 copies/ml,(3.590 ± 0.884) log10 copies/ml,(2.987 ± 0.673) log10 copies/ml and (2.933 ± 0.535) log10 copies/ml at 4,8,12 and 24 weeks.At 24 weeks,there were 28.6% patients achieved HBV DNA < 500 copies/ml in group ETV 1.0 mag,but there were 80.8% patients in group ETV + ADV achieved this level.Statistically significant difference existed between (x2 =8.469,P =0.004 ).At 48 weeks,there were still 4 patients achieved HBV DNA < 500 copies/ml in group ETV 1.0 mg,but patients in group ETV + ADV all achieved it.At 24weeks,ALT levels of 42.9% patients in group ETV 1.0 mg were back to normal,but there were 92.3% patients' ALT levels back to normal in group ETV + ADV.There was statistically significant difference ( x2 =9.337,P =0.002).At 48 weeks,ALT levels of 57.1% patients in group ETV 1.0 mg were back to normal,but all patients' ALT levels were back to normal in group ETV + ADV.At 48 weeks,there was 1 patient with HBeAg seroconversion in group ETV 1.0 mg while there were 4 patients in group ETV + ADV.Conclusion As rescue treatment for patients with chronic hepatitis B who had previously resisted LAM and failed with treatment of LAM + ADV,ETV + ADV was more efficient than ETV 1.0 mg monotherapy,and it can achieve better virological and biochemical response.
Keywords:Hepatitis B  chronic  Lamivudine  Adefovir dipivoxil  Entecavir
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