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首页> 外文期刊>Journal of viral hepatitis. >Hepatitis C virus free-virion and immune-complex dynamics during interferon therapy with and without ribavirin in genotype-1b chronic hepatitis C patients.
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Hepatitis C virus free-virion and immune-complex dynamics during interferon therapy with and without ribavirin in genotype-1b chronic hepatitis C patients.

机译:基因型1b慢性丙型肝炎患者使用或不使用利巴韦林的干扰素治疗期间的丙型肝炎病毒自由毒粒和免疫复合物动态。

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The Synergistic effect of interferon (IFN) and ribavirin for patients with chronic hepatitis C has been demonstrated, but ribavirin has no apparent direct antiviral effect against hepatitis C virus (HCV) when used as monotherapy. To elucidate the mechanism of ribavirin on enhanced HCV eradication when used in combination therapy, we investigated the serum HCV dynamics of free-virions (FV) and immune-complexes (IC) in genotype-1b infected patients treated with IFN-alpha2b alone (n = 11) or in combination with ribavirin (n = 15). Serum FV- and IC-HCV RNA were separated by immunoprecipitation using anti-human immunoglobulin and quantified serially using real-time detection polymerase chain reaction. At the first phase (day 0-2), the decline of FV- and IC-HCV RNA was similar between the two treatment groups. At the second phase (day 2-28), the decline of IC was significantly faster in patients treated with IFN plus ribavirin compared with IFN alone [exponential decay slope = 0.079 +/- 0.036 vs 0.048 +/- 0.027 log10/day, P = 0.0248; half-life = 81.1 +/- 21.4 vs 135.1 +/- 61.4 h, P = 0.0053], although the second phase FV-decline was not significantly different between the two treatment groups. The fast second phase decline of IC was associated with sustained virological response to therapy. These results suggest that ribavirin may modulate the humoral immune response against HCV and trigger a favourable response to IFN. In conclusion, analysis of early IC-HCV dynamics is useful for predicting the response to therapy and for understanding the mechanism of action of antiviral drugs in chronic hepatitis C patients.
机译:已证明干扰素(IFN)和利巴韦林对慢性丙型肝炎患者具有协同作用,但是当用作单一疗法时,利巴韦林对丙型肝炎病毒(HCV)没有明显的直接抗病毒作用。为了阐明利巴韦林在联合治疗中增强HCV根除的机制,我们调查了仅接受IFN-alpha2b治疗的基因型1b感染患者中游离病毒颗粒(FV)和免疫复合物(IC)的血清HCV动态变化(n = 11)或与利巴韦林联用(n = 15)。使用抗人免疫球蛋白通过免疫沉淀分离血清FV-和IC-HCV RNA,并使用实时检测聚合酶链反应进行系列定量。在第一阶段(第0-2天),两个治疗组之间FV-和IC-HCV RNA的下降相似。在第二阶段(第2-28天),与单独使用IFN相比,用IFN加利巴韦林治疗的患者IC的下降明显更快[指数衰减斜率= 0.079 +/- 0.036 vs 0.048 +/- 0.027 log10 /天,P = 0.0248;半衰期= 81.1 +/- 21.4 vs 135.1 +/- 61.4 h,P = 0.0053],尽管第二阶段FV下降在两个治疗组之间没有显着差异。 IC的快速第二阶段下降与对治疗的持续病毒学应答有关。这些结果表明利巴韦林可以调节针对HCV的体液免疫应答并引发对IFN的有利应答。总之,早期IC-HCV动态分析有助于预测慢性丙型肝炎患者对治疗的反应以及了解抗病毒药物的作用机制。

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