针对 La 自身抗原、NS5B 或 hVAP-A 的 siRNA 组合对抑制 HCV 复制具有叠加效应。

Hepatitis research and treatment Pub Date : 2016-01-01 Epub Date: 2016-06-29 DOI:10.1155/2016/9671031
Anirban Mandal, Krishna Kumar Ganta, Binay Chaubey
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引用次数: 0

摘要

丙型肝炎病毒是导致慢性肝炎、肝硬化和肝细胞癌等慢性肝病的主要原因。目前可用的直接作用抗病毒药物提高了成功率,但高昂的费用限制了它们的使用,尤其是在印度等发展中国家。在本研究中,我们评估了针对 HCV RNA 依赖性 RNA 聚合酶 NS5B 和细胞因子、La 自身抗原、PSMA7 和人类 VAMP 相关蛋白的几种 siRNA 的抗 HCV 潜力,以阻断病毒生命周期的不同步骤。这些靶基因被单独或组合下调,并评估了它们对病毒复制的影响。单独下调 La 自身抗原、PSMA7、hVAP-A 和 NS5B 可抑制 HCV 复制,抑制率分别为 67.2%、50.7%、39% 和 52%。然而,当多个基因同时被下调时,抗病毒效果更为明显。将针对 La 自身抗原的 siRNA 与 NS5B 或 hVAP-A 结合使用,能更有效地抑制 HCV 复制。我们的研究结果表明,siRNA 是一种抑制 HCV 复制的潜在治疗工具,同时针对多个病毒步骤的 siRNAs 组合比沉默单一靶点更有效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Combinations of siRNAs against La Autoantigen with NS5B or hVAP-A Have Additive Effect on Inhibition of HCV Replication.

Combinations of siRNAs against La Autoantigen with NS5B or hVAP-A Have Additive Effect on Inhibition of HCV Replication.

Combinations of siRNAs against La Autoantigen with NS5B or hVAP-A Have Additive Effect on Inhibition of HCV Replication.

Combinations of siRNAs against La Autoantigen with NS5B or hVAP-A Have Additive Effect on Inhibition of HCV Replication.

Hepatitis C virus is major cause of chronic liver diseases such as chronic hepatitis, liver cirrhosis, and hepatocellular carcinoma. Presently available direct-acting antiviral drugs have improved success rate; however, high cost limits their utilization, especially in developing countries like India. In the present study, we evaluated anti-HCV potential of several siRNAs targeted against the HCV RNA-dependent RNA polymerase NS5B and cellular factors, La autoantigen, PSMA7, and human VAMP-associated protein to intercept different steps of viral life cycle. The target genes were downregulated individually as well as in combinations and their impact on viral replication was evaluated. Individual downregulation of La autoantigen, PSMA7, hVAP-A, and NS5B resulted in inhibition of HCV replication by about 67.2%, 50.7%, 39%, and 52%, respectively. However, antiviral effect was more pronounced when multiple genes were downregulated simultaneously. Combinations of siRNAs against La autoantigen with NS5B or hVAP-A resulted in greater inhibition in HCV replication. Our findings indicate that siRNA is a potential therapeutic tool for inhibiting HCV replication and simultaneously targeting multiple viral steps with the combination of siRNAs is more effective than silencing a single target.

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