Chia Nan University of Pharmacy & Science Institutional Repository:Item 310902800/34869
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    標題: Development of NS2B-NS3 protease inhibitor that impairs Zika virus replication
    作者: Lin, Wen-Wei
    Huang, Yi-Jung
    Wang, Yen-Tseng
    Lin, Yun-Syuan
    Mazibuko, Nonsikelelo
    Chen, Chien-Shu
    Cheng, Tian-Lu
    Chang, Chih-Shiang
    Leu, Yu-Ling
    Chen, Chiao-Yun
    Chuang, Chih-Hung
    貢獻者: Kaohsiung Med Univ, Coll Med, Sch Post Baccalaureate Med, Dept Lab Med
    Kaohsiung Med Univ, Grad Inst Med, Coll Med
    Kaohsiung Med Univ, Drug Dev & Value Creat Res Ctr
    Kaohsiung Med Univ Hosp, Dept Med Res
    Kaohsiung Med Univ, Coll Med, Sch Post Baccalaureate Med, Dept Biochem
    Kaohsiung Med Univ, Dept Biomed Sci & Environm Biol
    China Med Univ, Sch Pharm
    China Med Univ, Drug Dev Ctr
    Chia Nan Univ Pharm & Sci, Dept Pharm
    Kaohsiung Med Univ Hosp, Dept Med Imaging
    Kaohsiung Med Univ, Coll Med, Sch Postbaccalaureate Med
    Kaohsiung Med Univ, Dept Med Lab Sci & Biotechnol
    Kaohsiung Med Univ, Dept Med Lab Sci & Biotechnol
    Kaohsiung Med Univ Hosp, Dept Med Imaging
    關鍵字: Zika virus (ZIKV)
    ZIKV NS2B-NS3 protease
    Small molecule inhibitor
    Non-competitive
    日期: 2023
    上傳時間: 2024-12-25 11:04:51 (UTC+8)
    出版者: ELSEVIER
    摘要: Zika virus (ZIKV) is a mosquito-borne flavivirus that causes severe neurological disorders, such as microcephaly in fetuses. Most recently, an outbreak of ZIKV started in Brazil in 2015. To date, no therapeutic agents have been approved to treat ZIKV infection in the clinic. Here, we screened a small molecule inhibitor that can inhibit the function of ZIKV non-structural protein 2B (NS2B)-NS3 protease (ZIKV NS2B-NS3 protease), thereby interfering with viral replication and spread. First, we identified the half maximal inhibitory concentration (IC50) of com-pound 3 (14.01 mu M), 8 (6.85 mu M), and 9 (14.2 mu M) and confirmed that they are all non-competitive inhibitors. In addition, we have used the blind molecular docking method to simulate the inhibition area of three non-competitive inhibitors (compound 3, 8, and 9) with the ZIKV NS2B-NS3 protease. The results indicated that the four allosteric binding residues (Gln139, Trp148, Leu150, and Val220) could form hydrogen bonds or non-bonding interactions most frequently with the three compounds. The interaction might induce the reaction center conformation change of NS2B-NS3 protease to reduce catalyzed efficiency. The concentration of compounds required to reduce cell viability by 50% (CC50), and the concentration of compounds required to inhibit virus-induced cytopathic effect by 50% (EC50) of three potential compounds are >200 mu M, 2.15 mu M (compound 3), > 200 mu M, 0.52 mu M (compound 8) and 61.48 mu M, 3.52 mu M (compound 9), and Temoporfin are 61.05 mu M, 2 mu M, respectively. To select candidate compounds for further animal experiments, we analyzed the selectivity index (SI) of compound 3 (93.02), 8 (384.61), 9 (17.46), and Temoporfin (30.53, FDA-approved drug against cancer). Compound 8 has the highest SI value. Therefore, compound 8 was selected for verification in animal models. In vivo, compound 8 significantly delayed ZIKV-induced lethality and illness symptoms and decreased ZIKV-induced weight loss in a ZIKV-infected suckling mouse model. We conclude that compound 8 is worth further investigation for use as a potential future therapeutic agent against ZIKV infection.
    關聯: Virus Research, v.329, Article 199092
    顯示於類別:[行政單位] 456

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