Identification of Peptide Leads to Inhibit Hepatitis C Virus: Inhibitory Effect of Plectasin Peptide Against Hepatitis C Serine Protease

被引:0
作者
Ammar Y. Abdulrahman
Hussin A. Rothan
Nurshamimi Nor Rashid
See Khai Lim
Wajihah Sakhor
Kah Ching Tee
Teow Chong Teoh
Noorsaadah A. Rahman
Rohana Yusof
机构
[1] University of Malaya,Department of Molecular Medicine, Faculty of Medicine
[2] University of Malaya,Faculty of Science, Institute of Biological Sciences
[3] University of Malaya,Department of Pharmacy, Faculty of Medicine
[4] University of Malaya,Department of Chemistry, Faculty of Science
来源
International Journal of Peptide Research and Therapeutics | 2017年 / 23卷
关键词
Antiviral peptide; Plectasin; Hepatitis C virus; NS3-4A serine protease; HCV replicon assay;
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中图分类号
学科分类号
摘要
The emerging of hepatitis C virus (HCV) resistant strains has been considered as a main drawback of the available drugs. Since HCV has a large inactive surface, we would like to hypothesis that the mutation occur in HCV is minimal and causing less resistance against inhibition. In this study, a short peptide inhibitor of HCV namely plectasin was identified by HCV NS3-4A serine protease assay. Plectasin peptide showed considerable inhibition against HCV NS3-4A serine protease. Enzymatic activity of the recombinant NS3-4Apro was analysed by fluorescence release from several fluorogenic peptide substrates which resembling the dibasic cleavage site sequences of the flavivirus polyprotein precursor. Of all amc-labelled peptides, Pyr-RTKR-amc was the most efficiently cleaved substrate with the lowest Km value of 20 µM. The kinetic assay showed that plectasin peptide inhibited NS3-4Apro activity with an IC50 value of 4.3 μM compared to the aprotinin as a standard proteases inhibitor with an IC50 of 6.1 μM. From the results, plectasin peptide also demonstrated a dose-dependent inhibition of HCV replication with a considerable reduction in RLuc activity at 15 µM using HCV replicon- containing Huh-7 cells. Our study has identified a unique natural peptide that can be used to highlight novel structures for the development of drug derivatives with high efficacy of HCV NS3-4A protease inhibitors.
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页码:163 / 170
页数:7
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