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    題名: Characterization of Trans- and Cis-Cleavage Activity of the SARS Coronavirus 3CLpro Protease: Basis for the in Vitro Screening of anti-SARS Drugs
    作者: 林振文(Lin Cheng Wen)*;蔡長海(Chang-Hai Tsai);蔡輔仁(Fuu-Jen Tsai);(Pei-Jer Chen);賴建成(Chien-Chen Lai);萬磊(Lei Wan);(Hua-Hao Chiu);(Kuan-Hsun Lin)
    貢獻者: 健康照護學院醫學檢驗生物技術學系;中國附醫檢驗醫學部
    關鍵詞: SARS-coronavirus;3C-like protease;trans- and cis-cleavage;Substrate specificity
    日期: 2004-09
    上傳時間: 2009-08-20 18:28:59 (UTC+8)
    摘要: Severe acute respiratory syndrome (SARS) has been globally reported. A novel coronavirus (CoV), SARS-CoV, was identified as the etiological agent of the disease. SARS-CoV 3C-like protease (3CLpro) mediates the proteolytic processing of replicase polypeptides 1a and 1ab into functional proteins, playing an important role in viral replication. In this study, we demonstrated the expression of the SARS-CoV 3CLpro in Escherichia coli and Vero cells, and then characterized the in vitro trans-cleavage and the cell-based cis-cleavage by the 3CLpro. Mutational analysis of the 3CLpro demonstrated the importance of His41, Cys145, and Glu166 in the substrate-binding subsite S1 for keeping the proteolytic activity. In addition, alanine substitution of the cleavage substrates indicated that Gln-P1 in the substrates mainly determined the cleavage efficiency. Therefore, this study not only established the quantifiable and reliable assay for the in vitro and cell-based measurement of the 3CLpro activity, but also characterized the molecular interaction of the SARS-CoV 3CLpro with the substrates. The results will be useful for the rational development of the anti-SARS drugs.
    關聯: FEBS LETTERS574(1-3):131~137
    顯示於類別:[醫學檢驗生物技術學系暨碩士班 ] 期刊論文

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