慢性乙型肝炎恩替卡韦经治后联合长效干扰素的疗效预测分析

摘要/Abstract

摘要： 目的分析我院恩替卡韦经治的慢性乙型肝炎患者联合聚乙二醇干扰素α-2a治疗的疗效及探讨预测疗效的相关指标。方法选取恩替卡韦治疗至少1年且HBV DNA阴性的慢性乙型肝炎患者,予恩替卡韦联合聚乙二醇干扰素α-2a治疗48周或延长至72周,观察至96周。结果共纳入35例患者,分为两组,基线HBeAg阳性组(18例)、HBeAg阴性组(17例),两组基线指标差别无统计学意义。3例因不良反应退出研究,10例干扰素延长至72周。所有患者HBsAg消失率和HBsAg血清学转换率均为:48周时1/32(3.1%)和0/32(0)、72周时2/32(6.3%)和2/32(6.3%)、96周时3/32(9.4%)和2/32(6.3%);48、72、96周时HBsAg<1 IU/mL患者的比率分别为:6/32(18.8%)、8/32(25.0%)、6/32(18.8%)。24、48、72、96周时 HBsAg下降比率[HBsAg下降比率=(基线HBsAg-第疗程周HBsAg)/基线HBsAg]分别为:53.5%、83.8%、68.4%、62.5%。HBeAg阴性组较HBeAg阳性组的HBsAg消失率、HBsAg转换率、HBsAg下降比率均较高,但差别无统计学意义。基线、24周、48周HBsAg水平判断48周、96周时是否达到HBsAg清除、HBsAg<1 IU/mL、HBsAg<10 IU/mL的ROC曲线的曲线下面积平均值为0.927,有较高的预测价值。 ROC曲线分析:基线HBsAg<1 312 IU/mL,取得48周、96周HBsAg<1 IU/mL的概率大于0;第24周HBsAg<201 IU/mL时,取得48周HBsAg<10 IU/mL及96周HBsAg清除的概率大于0;第48周HBsAg<7.25 IU/mL时,取得96周HBsAg清除的概率大于0。基线HBsAg<1 500 IU/mL的患者,第24周HBsAg<200 IU/mL的比率达80%,这些患者HBsAg清除率和HBsAg转换率分别为:48周时1/12(8.3%)和0/12(0)、96周时3/12(25.0%)和2/12(16.7%),48周、96周HBsAg<1 IU/mL比率均为6/12(50.0%)。48周、96周HBsAg下降比率高达99.6%、99.2%。结论对于恩替卡韦经治慢性乙型肝炎,无论基线HBeAg阳性还是HBeAg阴性,可考虑联合干扰素治疗以期提高HBsAg血清学应答率,甚至实现临床治愈目标。基线HBsAg水平较低的患者属于优势人群,24周时HBsAg<200 IU/mL是取得较好HBsAg下降结果的预测因素,根据应答指导治疗,制定个体化精准治疗方案,有助于提高疗效。

关键词: 慢性乙型肝炎, 干扰素, 联合治疗, 临床治愈

Abstract: Objective To analyze the curative effect of adding peginterferon α-2a to entecavir (ETV) for the treatment of chronic hepatitis B (CHB) patients and to explore the related indexes for the prediction of clinical cure.Methods Patients with CHB who had received ETV for at least one year and achieved HBV DNA negative were selected and treated with ETV in combination with peginterferon α-2a for 48 weeks, or extended the treatment to 72 weeks with a prolonged observation duration of 96 weeks. The HBsAg reduction ratio [(Baseline HBsAg- HBsAg in the Follow-up period of Treatment)/Baseline HBsAg] was calculated as a judgement of treatment efficacy.Results A total of 35 patients were included and divided into two groups, baseline HBeAg positive group (N=18 cases) and baseline HBeAg negative group (N=17 cases). There was no significant difference in baseline parameters between the two groups. Three patients withdrew from the study due to side effects, and 10 patients received interferon for 72 weeks. The HBsAg disappearance rates and HBsAg seroconversion rates of all patients were 1/32 (3.1%) and 0/32 (0) at week 48, 2/32 (6.3%),2/32 (6.3%) at week 72, 3/32 (9.4%),and 2/32 (6.3%) at week 96. At week 48, 72 and 96, the rates of HBsAg<1 IU/mL were 6/32 (18.8%), 8/32 (25.0%) and 6/32 (18.8%), respectively. At week 24, 48, 72 and 96, the medians of the HBsAg reduction ratios were 53.5%, 83.8%, 68.4% and 62.5%, respectively. When compared with the baseline HBeAg positive group, the HBsAg disappearance rate, HBsAg seroconversion rate, HBsAg reduction ratio in the baseline HBeAg negative group were all higher, but without significant difference. The average area under the receiver operating characteristic curve (ROC) for using the HBsAg levels at baseline, Week 24, Week 48 to predict HBsAg clearance, HBsAg<1 IU/mL and HBsAg<10 IU/mL at 48 weeks and 96 weeks was 0.927, which had a high predictive value. According to the analysis of ROC curve coordinates, when the baseline HBsAg was less than 1312 IU/mL, the probability of HBsAg<1 IU/mL at Week 48 and 96 was higher than zero; when the HBsAg level was less than 201 IU/mL at Week 24, the probability of HBsAg<10 IU/mL at Week 48 and HBsAg clearance at Week 96 was higher than zero; when the HBsAg level was less than 7.25 IU/mL at Week 48, the probability of HBsAg clearance at Week 96 was higher than zero. For the preponderant patients with baseline HBsAg<1500 IU/mL, the rate of patients with HBsAg<200 IU/mL at Week 24 was as high as 80%. For patients with baseline HBsAg<1 500 IU/mL and HBsAg<200 IU/mL at Week 24, the HBsAg clearance rates and HBsAg conversion rates were 1/12(8.3%) and 0/12(0) at Week 48, 3/12(25.0%) and 2/12(16.7%) at Week 96 respectively. The rates of patients with HBsAg<1 IU/mL at Week 48 and 96 were all 6/12(50.0%). The HBsAg reduction ratios were as high as 99.6% and 99.2% at Week 48 and 96, respectively.Conclusion No matter HBeAg positive or negative, a combined interferon therapy should be considered in CHB patients treated by entecavir to improve HBsAg serological response rate and even reach the goal of clinical cure. Patients with low HBsAg level (less than 1 500 U/mL) were the advantageous population. HBsAg<200 IU/mL at Week 24 of the combined therapy was a predictive factor for a better HBsAg decline. It is advocated to apply individualized treatment regime to CHB patients formulated by their response in order to achieve a clinical curative effect.

Key words: Chronic hepatitis B, Interferons, Combination therapy, HBsAg reduction ratio, Clinical cure

林彬彬, 肖志鸿, 王菲, 阮清发, 汤钰菁, 欧阳丽娟. 慢性乙型肝炎恩替卡韦经治后联合长效干扰素的疗效预测分析[J]. 肝脏, 2021, 26(1): 27-32.

LIN Bin-bin, XIAO Zhi-hong, WANG Fei, RUAN Qing-fa, TANG Yu-jing, OUYANG Li-juan. A predictive analysis for the therapeutic effect of adding peginterferon to entecavir on chronic hepatitis B patients[J]. Chinese Hepatolgy, 2021, 26(1): 27-32.

参考文献

[1] 王贵强,王福生,成军,等. 慢性乙型肝炎防治指南(2015年版). 中国肝脏病杂志(电子版),2015,03:1-18.
[2] Ning Q,Han MF, Sun YT,et al. Switching from entecavir to PegIFN alfa-2a in patients with HBeAg-positive chronic hepatitis B: a randomised open-label trial (OSST trial). J Hepatol,2014,61:777-784.
[3] Hu P,Jia S,Zhang W,et al. A multi-center randomized study on the efficacy and safety of switching to peginterferon alpha-2a (40KD) for 48 or 96 weeks in HBeAg positive CHB patients with a prior NUC history for 1 to 3 years: an interim analysis of NEW SWITCH study. Hepatology,2014,60:1273a-1274a.
[4] Li GJ,Yu YQ,Chen SL,et al. Sequential combination therapy with pegylated interferon leads to loss of hepatitis B surface antigen and hepatitis B e antigen (HBeAg) seroconversion in HBeAg-positive chronic hepatitis B patients receiving long-term entecavir treatment. Antimicrob. Agents Chemother,2015,59:4121-4128.
[5] Brouwer WP,Xie Q,Sonneveld MJ,et al. Adding pegylated interferon to entecavir for hepatitis B e antigen-positive chronic hepatitis B: A multicenter randomized trial (ARES study). Hepatology,2015,61(5):1512-1522.
[6] Tamaki N,Kurosaki M,Kusakabe A,et al. Hepatitis B surface antigen reduction by switching from long-term nucleoside/nucleotide analogue administration to pegylated interferon. J Viral Hepat,2017,24:672-678.
[7] 贾继东,李兰娟. 慢性乙型肝炎防治指南(2010年版). 肝脏,2011(1):2-16.
[8] 陈新月,柳雅立. 慢性乙型肝炎患者如何获得临床治愈. 实用肝脏病杂志,2016(3):257-260.
[9] Liu J,Lee MH,Batrla-Utermann R,et al. A predictive scoring system for the seroclearance of HBsAg in HBeAg-seronegative chronic hepatitis B patients with genotype B or C infection. J Hepatol,2013,58:853-860.
[10] Tseng TC,Liu CJ,Su TH,et al. Serum hepatitis B surface antigen levels predict surface antigen loss in hepatitis B e antigen seroconverters. Gastroenterology,2011,141:517-525.
[11] Patrick M,Ferruccio B,Cihan Y,et al. Hepatitis B surface antigen levels: association with 5-year response to peginterferon alfa-2a in hepatitis B e-antigen-negative patients. Hepatol Int,2013,7:88-97.
[12] Liaw YF,Jia JD,Chan HLY,et al. Shorter durations and lower doses of peginterferon alfa-2a are associated with inferior hepatitis B e antigen seroconversion rates in hepatitis B virus genotypes B or C. Hepatology,2011,54:1591-1599.
[13] Teerha P,Patrick M,Matei P,et al. Hepatitis B surface antigen: association with sustained response to peginterferon alfa-2a in hepatitis B e antigen-positive patients. Hepatol Int,2013,7:429-436.

[1]	许俊, 谢国艳, 黄敏. 慢性乙型肝炎患者血清可溶性E-钙黏蛋白表达与氧化应激的相关性分析[J]. 肝脏, 2021, 26(1): 19-21.
[2]	冯少阳, 李广明, 苏航. 瞬时弹性成像对慢性乙型肝炎合并非酒精性脂肪性肝病患者肝纤维化的评估价值[J]. 肝脏, 2021, 26(1): 44-46.
[3]	赵海东, 陈灵峰, 林巧欣, 李艺芳. 聚乙二醇干扰素α短期治疗HBsAg水平极低的非活动性HBsAg携带者的疗效观察[J]. 肝脏, 2020, 25(9): 937-939.
[4]	高文, 杨雪, 窦爱华, 惠威, 刘梅, 徐斌, 段钟平. 维生素D缺乏对乙型肝炎患者的影响[J]. 肝脏, 2020, 25(9): 940-942.
[5]	沙尼亚·尼亚孜, 柯比努尔·吐尔逊, 潘珂君, 孙晓风. 长效干扰素 α-2b联合阿德福韦酯或恩替卡韦治疗耐药HBeAg阳性乙型肝炎疗效及安全性比较[J]. 肝脏, 2020, 25(7): 746-748.
[6]	周莹, 杨俊梅, 张桂珍, 甄明慧. 学龄前HBeAg阴性慢性乙型肝炎患儿临床特点分析[J]. 肝脏, 2020, 25(6): 605-606.
[7]	吴智慧, 丁媛. 慢性乙型肝炎肝硬化患者恩替卡韦抗病毒干预后肝脏弹性成像定量变化观察[J]. 肝脏, 2020, 25(6): 630-632.
[8]	贺尼娅, 王琳. 慢性乙型肝炎患者血清胆固醇与肝纤维化的相关性研究[J]. 肝脏, 2020, 25(6): 645-647.
[9]	钟大明, 蓝柏钊, 欧超兰, 陈开革, 温静, 李嘉丽, 周甦, 莫穆隆, 梁柱石. HBsAg不同载量的HBeAg阳性慢性乙型肝炎对恩替卡韦治疗应答比较[J]. 肝脏, 2020, 25(5): 505-507.
[10]	孙蔚, 杨星. 瞬时弹性成像和声脉冲辐射力成像技术诊断慢性乙型肝炎肝纤维化的价值[J]. 肝脏, 2020, 25(5): 534-535.
[11]	卢君瑶, 王登宇, 尹东林, 白玉盘, 许洁. HBV相关肝细胞癌的临床特征及危险因素分析[J]. 肝脏, 2020, 25(3): 285-287.
[12]	沈张平, 王钦君, 季沈杰. 血清miR127-3P与原发性肝癌的相关性研究[J]. 肝脏, 2020, 25(3): 302-305.
[13]	薛宏丽. HBsAg定量在慢性乙型肝炎治疗中的意义[J]. 肝脏, 2020, 25(3): 308-310.
[14]	梅栖榕, 杨丽, 沈毅. 慢性乙型肝炎患者长期服用阿德福韦酯与肾性低磷血症的相关性[J]. 肝脏, 2020, 25(3): 311-313.
[15]	孔媛媛, 魏巍, 单姗, 马红, 欧晓娟, 徐小元, 段钟平, 侯金林, 魏来, 尤红, 贾继东, 中国消除乙肝临床科研平台(CR-HepB)研究组. 乙型肝炎肝硬化患者的临床特征与抗病毒治疗模式变化[J]. 肝脏, 2020, 25(2): 123-127.