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目的：探究在 e 抗原（ HBeAg）阳性的慢性乙型肝炎患者采用聚乙二醇干扰素 -2a (peg-2a)联合核苷类药物治疗过程中，加用胸腺五肽对细胞免疫应答的影响。方法：选择采用聚乙二醇干扰素alpha-2a 联合核苷类药物（拉米夫定 + 阿德福韦酯）治疗 48 周， HBeAg 仍为阳性，且 HLA-A2 阳性的慢性乙型肝炎患者 18 例，分为两组。一组原方案延长联合治疗作为对照，另一组在原方案基础上再加用胸腺五肽治疗（ 1 0 mg/ 次， 2 次 / 周，共 24 周）治疗，所有病人均治疗至 96 周。并做体外 HBV 特异性细胞毒 T 淋巴细胞(HBV specific CTL)培养增殖，通过 Elispot 技术分析其分泌细胞因子（肿瘤坏死因子 -alpha，干扰素 -r，白介素 -10)的功能。结果： HBeAg 转阴率，治疗 96 周时联合胸腺五肽组为 44.4 %（ 4 /9），原方案对照组为 22.2 %（ 2 /9）。 HBsAg 滴度， 48 周时， HBsAg 为 4571± 3772 IU/m:； 96 周时，联合胸腺五肽组为 1 962± 2869 IU/mL，转阴 1 人，原方案对照组为 3490± 3124 IU/mL， P=0.093。 HBV 特异性 CTL 培养增殖， 96 周时联合胸腺五肽组高于原方案对照组，且联合胸腺五肽组 TNF- 的分泌也高于原方案对照组， P<0. 05 。结论：胸腺五肽显著增强干扰素抗病毒治疗过程中的特异性 CTL 效应。

英文摘要:

Objective:To investigate whether Thymopentin 5 (TP5) affects cellular immune during interferon antiviral therapy in HBeAg-positive chronic hepatitis B patients.Methods:1 8 patients didn't achieve HBeAg seroconversion after peginterferon alpha-2a combined with lamivudine and adefovir dipivoxil for 48 weeks. They were randomly divided into two groups including continuing interferon based combination therapy with (n=9) or without (n=9) TP5 (10 mg, twice a week for 24 weeks) till 96 weeks. We conduct in vitro HBV specific CTL cultures and proliferation assays, HBcAg-induced cytokine secretion (INF-r, TNF-alpha, IL-1 0).Results:In TP5 administrated group, the rate of HBeAg seroconversion was 44.4 %(4/9), mean HBsAg level was 1 962± 2869 IU/mL. In control group, the rate of HBeAg seroconversion was 22.2 % (2 /9), mean HBsAg level was 3490± 3124 IU/mL. Proliferative response ofHBV specific CTL in TP5 administrated group was relatively strong at week 96. TNF-alpha production also increased at week 96 in TP5 administrated group, as compared to control group.Conclusion:Thymopentin 5 significantly enhanced the HBV-specific CTL reactivity in interferon antiviral therapy

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