不同转换治疗策略对经治的低病毒血症慢性乙型肝炎患者疗效的影响:单中心回顾性研究*

doi:10.3969/j.issn.1672-5069.2022.05.007

摘要/Abstract

摘要： 目的探讨不同转换治疗策略对慢性乙型肝炎(CHB)经治发生低病毒血症(LLV)患者疗效的影响。方法本研究纳入197例ETV或TDF经治的发生LLV的CHB患者,被分为A组74例,B组63例和C组60例,分别给予ETV或TDF单药维持治疗或TAF替换治疗或ETV或TDF联合长效干扰素(peg-IFN)α-2b治疗观察48周。结果在48周治疗末,C组完全病毒学应答率(CVR)和HBeAg阴转率分别为90.0%和41.7%,显著高于A组的16.2%和5.4%(P<0.05)或B组的66.7%和9.5%(P<0.05),B组和C组血清ALT复常率分别为20.6%和23.3%,显著高于A组的8.1%(P<0.05);C组血清HBsAg水平为3.0(2.8,3.4)lgIU/ml,显著低于A组【3.3(2.9,3.9)lgIU/ml,P<0.05】或B组【3.4(3.3,3.8)lgIU/ml,P<0.05】,血清HBeAg水平为0.1(-0.7,0.0)lgIU/ml,显著低于A组【0.6(-0.6,1.8) lgIU/ml,P<0.05】或B组【0.6(-0.3,1.8)lgIU/ml,P<0.05】,血清HBV DNA水平为1.3(1.3,1.3)lgIU/ml,显著低于A组【1.7(1.3,2.0)lgIU/ml,P<0.05】或B组【1.6(1.3,1.4)lgIU/ml,P<0.05】;B组和C组肝脏硬度检测(LSM)分别为6.4(4.3,8.4) kPa和6.2(4.2,7.7) kPa,显著低于A组【8.6(5.2,10.7) kPa,P<0.05】,三组血清ALT水平比较,无统计学差异(P＞0.05)。结论对于核苷类经治出现LLV的CHB患者,为保险起见,换用TAF或继续核苷类联合peg-IFNα-2b治疗可进一步获得较好的病毒学应答率和一定程度的血清学应答率,其对长期疾病转归的影响还需要观察。

关键词: 慢性乙型肝炎, 低病毒血症, 富马酸丙酚替诺福韦, 聚乙二醇干扰素α-2b, 转换治疗

Abstract: Objective The aim of this study was to investigate the efficacy of switching from entecavir(ETV) or tenofovir(TDF) to other different antiviral therapy in ETV- or TDF-treated chronic hepatitis B (CHB) patients with low-level viraemia (LLV). Methods A total of 197 patients with CHB who had been treated with ETV or TDF were enrolled in this study and were divided into group A (n=74) continuing ETV or TDF treatment, group B( n=63) switching to TAF therapy and group C (n= 60) switching to ETV or TDF and peg-IFNα-2b combination therapy. The regimen lasted for (48±2) weeks. Results At the end of 48 week treatment, the complete virologic response and serum HBeAg negative rates in group C were 90.0% and 41.7%, significantly higher than 16.2% and 5.4%(P<0.05) in group A or 66.7% and 9.5%(P<0.05) in group B, and serum ALT normalization rates in group B and group C were 20.6% and 23.3%, significantly higher than 8.1%(P<0.05) in group A; serum HBsAg level in group C was 3.0(2.8, 3.4)lgIU/ml, significantly lower than [3.3(2.9, 3.9)lgIU/ml, P<0.05] in group A or [3.4(3.3, 3.8)lgIU/ml, P<0.05] in group B, serum HBeAg level was 0.1(-0.7, 0.0)lgIU/ml, significantly lower than [0.6(-0.6, 1.8) lgIU/ml, P<0.05] in group A or [0.6(-0.3, 1.8)lgIU/ml, P<0.05] in group B, and serum HBV DNA load was 1.3(1.3, 1.3)lgIU/ml, significantly lower than [1.7(1.3, 2.0)lgIU/ml, P<0.05] in group A or [1.6(1.3, 1.4)lgIU/ml, P<0.05] in group B; the LSMs in group B and group C were 6.4(4.3, 8.4) kPa and 6.2(4.2, 7.7) kPa, both significantly lower than [8.6(5.2, 10.7) kPa, P<0.05] in group A, and serum ALT levels in the three groups were not significantly different (P＞0.05). Conclusion The switch to TAF or combined with peg-IFNα-2b therapy in ETV- or TDF-treated patients with LLV might benefit for further virologic and even serologic response, and warrants clinical investigation.

Key words: Hepatitis B, Low-level viremia, Tenofovir disoproxil fumarate, Peg-interferon α-2b, Switching therapy

王玉珊, 孔银, 刘元元, 刘天府, 麻爱娣, 张亚萍, 李永芳, 张岭漪. 不同转换治疗策略对经治的低病毒血症慢性乙型肝炎患者疗效的影响:单中心回顾性研究^*[J]. 实用肝脏病杂志, 2022, 25(5): 633-636.

Wang Yushan, Kong Yin, Liu Yuanyuan, et al.. Different switching therapy for chronic hepatitis B patients with low-level viraemia : a single-center retrospective study[J]. Journal of Practical Hepatology, 2022, 25(5): 633-636.

参考文献

[1]Du Jeong I, Jung S W, Park B R, et al. Clinicalcourse of partial virologic response with prolonged tenofovir therapy in nuclos(t)ides-nave patients with chronic hepatitis B. Dig Dis Sci, 2017, 62(10):2908-2914.
[2]Lovett G C, Nguyen T, Iser D M, et al. Efficacy and safety of tenofovir in chronic hepatitis B: Australian real world experience. World J Hepatol, 2017, 9(1):48-56.
[3]Okuda CH. Challenges of hepatitis B in the era of antiviral therapy. J Gastroenterol Hepatol, 2018, 34(3):501-506.
[4]Sun Y, Wu X, Zhou J, et al. Persistent low level of hepatitis B virus promotes fibrosis progression during therapy. Clin Gastroenterol H, 2020, 18(11):2582-2591.
[5]路正昭, 孙亚朦, 尤红. 慢性乙型肝炎低病毒血症致肝纤维化与肝细胞癌. 中华肝脏病杂志,2021, 29(12):1144-1146.
[6]Nam J Y, Chang Y, Cho H, et al. Delayed viral suppression during antiviral therapy is associated with increased hepatocellular carcinoma rates in HBeAg-positive high viral load chronic hepatitis B. J Viral Hepat, 2018, 25(5):552-560.
[7]Kim J H, Sinn D H, Kang W, et al. Low-level viremia and the increased risk of hepatocellular carcinoma in patients receiving entecavir treatment. Hepatology, 2017, 66(2): 335-343.
[8]Terrault N A, McMahon B J, Chang K M, et al. Update on prevention, diagnosis, and treatment of chronic hepatitis B: AASLD 2018 hepatitis B guidance. Clin Liver Dis, 2018, 67(4):1560-1599.
[9]中华医学会感染病学分会, 中华医学会肝病学分会. 慢性乙型肝炎防治指南(2019年版). 实用肝脏病杂志, 2020, 23(1):9-32.
[10] 中国肝炎防治基金会, 中华医学会感染病学分会, 中华医学会肝病学分会和中国研究型医院学会肝病专业委员会. 瞬时弹性成像技术诊断肝纤维化专家共识(2018年更新版). 中华肝脏病杂志, 2019, 27(3):182-191.
[11] 鲁凤民, 封波, 郑素军, 等. 核苷(酸)类似物经治的慢性乙型肝炎患者低病毒血症的研究现状. 临床肝胆病杂志, 2021, 37(6): 1268-1274.
[12] Song J E, Lee C H, Kim B S. Efficacy of long-term tenofovir disoproxil fumarate therapy in chronic hepatitis B patients with partial virologic response in real practice. Korean J Intern Med, 2019, 34(4): 802–810.
[13] Cho J Y, Sohn W, Sinn D H,et al. Long-term real-world entecavir therapy in treatment-nave hepatitis B patients: base-line hepatitis B virus DNA and hepatitis B surface antigen levels predict virologic response. Korean J Intern Med, 2017, 32(4):636-646.
[14] Wong L H , Wong W S , Chan H Y , et al. Undetectable HBV DNA at month 12 ofentecavir treatment predicts maintained viral suppression and HBeAg-seroconversion in chronic hepatitis B patients at 3 years. Aliment Pharm Ther, 2012, 35(11):1326-1335.
[15] Yim H J, Kim I H, Suh S J, et al. Switching to tenofovir vs continuingentecavir for hepatitis B virus with partial virologic response to entecavir: a randomized controlled trial. J Viral Hepat, 2018, 25(11):1321-1330.
[16] Wang Y H, Liao J, Zhang D M, et al. Tenofovir monotherapy versus tenofovir plusentecavir combination therapy in HBeAg-positive chronic hepatitis patients with partial virological response to entecavir. J Med Virol, 2020, 92(3):302-308.
[17] Nguyen M H, Atsukawa M, Ishikawa T, et al. Outcomes ofsequential therapy with tenofovir alafenamide after long-term entecavir. Am J Gastroenterol, 2021, 116(6):1264-1273.
[18] Ogawa E, Nomura H, Nakamuta M, et al. Tenofovir alafenamide after switching from entecavir or nucleos(t)ide combination therapy for patients with chronic hepatitis B. Liver Int, 2020, 40(7):1578-1589.
[19] Li Z B, Li L, Niu X X, et al. Switching from entecavir to tenofovir alafenamide for chronic hepatitis B patients with low-level viraemia. Liver Int, 2021, 41(6):1254-1264.
[20] 中华医学会肝病学分会. 扩大慢性乙型肝炎抗病毒治疗的专家意见. 中华肝脏病杂志, 2022, 30(2): 131-136.
[21] Hudu S A, Niazlin M T, Nordin S A, et al. Quantitativehepatitis B e antigen: a better predictor of hepatitis B virus DNA than quantitative hepatitis B surface antigen. Clin Lab, 2018, 64(4):443-449.
[22] 曹辉, 张玮. 核苷(酸)类药物治疗慢性乙型肝炎患者影响HBeAg血清转换的免疫学因素研究进展. 实用肝脏病杂志, 2017, 20(3):372-376.

不同转换治疗策略对经治的低病毒血症慢性乙型肝炎患者疗效的影响:单中心回顾性研究^*

Different switching therapy for chronic hepatitis B patients with low-level viraemia : a single-center retrospective study

PDF (PC)

可视化

摘要/Abstract

引用本文

使用本文

参考文献

相关文章 15

编辑推荐

Metrics

本文评价

[1]	徐欢, 谭钧元, 黄荷, 董丹丹. 聚乙二醇干扰素α-2a联合恩替卡韦治疗慢性乙型肝炎患者疗效及其外周血单个核细胞TLR4和B7-H1表达变化^*[J]. 实用肝脏病杂志, 2022, 25(5): 637-640.
[2]	王春莹, 屈耀宁, 乔炜, 刘静静, 胡颖辉. 恩替卡韦治疗慢性乙型肝炎患者血清HBV cccDNA和HBV pgRNA水平变化^*[J]. 实用肝脏病杂志, 2022, 25(5): 641-644.
[3]	贾婷, 李俊义, 张秀灵, 高斯媛, 杨婧, 杨晓冬. 恩替卡韦联合聚乙二醇干扰素α-2b治疗低水平血清HBsAg阳性的慢性乙型肝炎患者疗效研究^*[J]. 实用肝脏病杂志, 2022, 25(4): 488-491.
[4]	刘雨莹, 张娇珍, 周海娟, 潘芳蝶, 黎才丽, 钟昌宝. 替诺福韦治疗不同HBV基因型慢性乙型肝炎患者疗效研究^*[J]. 实用肝脏病杂志, 2022, 25(4): 492-495.
[5]	汤磊, 彭蕾, 叶珺, 张振华, 邹桂舟. 影响慢性乙型肝炎患者进展为肝硬化的多因素分析^*[J]. 实用肝脏病杂志, 2022, 25(4): 538-541.
[6]	黄俊榕, 吴昌儒, 吴健林. 恩替卡韦联合甘草酸二铵治疗慢性乙型肝炎患者效果研究^*[J]. 实用肝脏病杂志, 2022, 25(3): 327-330.
[7]	邹东花, 秘建威, 李玉苓, 赵森. 阿德福韦酯分别联合恩替卡韦或替诺福韦治疗rtA181V/T单位点突变的慢性乙型肝炎患者疗效初步研究^*[J]. 实用肝脏病杂志, 2022, 25(3): 331-334.
[8]	罗珂, 丁莉, 刘美. 慢性乙型肝炎患者血清miR-21和miR-148b水平变化及其预测肝组织炎症分级和纤维化分期价值探讨^*[J]. 实用肝脏病杂志, 2022, 25(3): 335-338.
[9]	王广丽, 徐欢, 董丹丹, 黄荷. 慢性乙型肝炎患者血清HBV恩替卡韦耐药基因突变模式调查^*[J]. 实用肝脏病杂志, 2022, 25(3): 339-342.
[10]	严兆兰, 祖红梅, 蔡长霞, 魏巍. 血清低水平丙氨酸氨基转移酶的HBV感染者临床特征分析^*[J]. 实用肝脏病杂志, 2022, 25(3): 343-346.
[11]	李春花, 李忠新, 张春雷, 曾学辉, 陈甜甜, 宋林立. 不同肝纤维化程度的慢性乙型肝炎患者血清FGF-21、PDGF-BB和FBRS水平变化及其临床意义探讨^*[J]. 实用肝脏病杂志, 2022, 25(3): 347-350.
[12]	姜悦萌, 马于琪, 阚春明, 尹华发. 应用核苷(酸)类治疗慢性乙型肝炎患者早期肾功能的变化^*[J]. 实用肝脏病杂志, 2022, 25(3): 351-354.
[13]	杨艳, 刘婷, 戴琳, 努丽曼姑·麦麦提, 刘环. 声触诊弹性成像检测肝脾硬度诊断慢性乙型肝炎患者肝纤维化效能分析^*[J]. 实用肝脏病杂志, 2022, 25(2): 183-186.
[14]	黄平, 曾霞, 张亚萍, 毛加丽. 肝静脉波形分型联合肝脏超声半定量评分对慢性乙型肝炎患者肝纤维化程度评估价值研究^*[J]. 实用肝脏病杂志, 2022, 25(2): 187-190.
[15]	李振, 宁姗姗, 郭影, 王甜甜, 李莉华, 叶美红, 宋源源. 慢性乙型肝炎患者肝组织LXRα和CYP7A1基因水平变化及其与肝组织炎症和纤维化程度的关系研究^*[J]. 实用肝脏病杂志, 2022, 25(2): 191-194.