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Small molecule inhibitors of the SARS-CoV Nsp15 endoribonuclease

机译:SARS-CoV Nsp15核糖核酸内切酶的小分子抑制剂

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The severe acute respiratory syndrome (SARS) virus encodes several unusual RNA processing enzymes, including Nsp15, an endoribonuclease that preferentially cleaves 3’ of uridylates through a ribonuclease A (RNase A)-like mechanism. Crystal structures of Nsp15 confirmed that the Nsp15 active site is structurally similar to that of RNase A. These similarities and our molecular docking analysis lead us to hypothesize that previously characterized RNase A inhibitors will also inhibit the SARS-CoV Nsp15. Benzopurpurin B, C-467929, C-473872, N-306711, N-65828, N-103019 and congo red were tested for effects on Nsp15 endoribonuclease activity. A fluorescence assay revealed that the IC50 values for inhibiting endoribonuclease activity were between 0.2 μM and 40 μM. These compounds were demonstrated to bind SARS-CoV Nsp15 by a differential scanning fluorimetry assay. Benzopurpurin B also inhibited the endoribonuclease activities of the Nsp15 orthologs from two other coronaviruses: mouse hepatitis virus (MHV) and infectious bronchitis virus (IBV). Benzopurpurin B, C-473872, and congo red reduced infectivity of MHV in L2 cells by 8- to 26- fold. The more effective drugs caused a decrease in MHV RNA accumulation. All three compounds reduced the infectivity of the SARS-CoV in Vero cells.
机译:严重急性呼吸系统综合症(SARS)病毒编码几种异常的RNA处理酶,包括Nsp15,这是一种内切核糖核酸酶,可通过类似核糖核酸酶A(RNase A)的机制优先切割尿嘧啶的3'。 Nsp15的晶体结构证实Nsp15活性位点在结构上与RNase A相似。这些相似性和我们的分子对接分析使我们推测,先前鉴定的RNase A抑制剂也将抑制SARS-CoV Nsp15。测试了苯并嘌呤B,C-467929,C-473872,N-306711,N-65828,N-103019和刚果红对Nsp15核糖核酸内切酶活性的影响。荧光分析表明,抑制核糖核酸内切酶活性的IC 50 值为0.2μM至40μM。通过差示扫描荧光测定法证明这些化合物结合SARS-CoV Nsp15。苯并嘌呤B还可抑制其他两种冠状病毒Nsp15直系同源物的核糖核酸内切酶活性:小鼠肝炎病毒(MHV)和传染性支气管炎病毒(IBV)。苯并嘌呤B,C-473872和刚果红将LHV细胞在L2细胞中的感染力降低了8到26倍。更有效的药物导致MHV RNA积累减少。所有这三种化合物均降低了Vero细胞中SARS-CoV的感染性。

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