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Structure-Property Relationship Studies of Influenza A Virus AM2-S31N Proton Channel Blockers

机译:流感病毒AM2-S31N质子通道阻挡机的结构 - 性质关系研究

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Majority of current circulating influenza A viruses carry the S31N mutation in their M2 genes, rendering AM2-531N as a high profile antiviral drug target. With our continuous interest in developing AM2-531N channel blockers as novel antivirals targeting both oseltamivir-sensitive and -resistant influenza A viruses, we report herein the structure-property relationship studies of AM2-S31N inhibitors. The goal was to identify lead compounds with improved microsomal stability and membrane permeability. Two lead compounds, 10d and 10e, were found to have high mouse and human liver microsomal stability (T-1/2, 145 min) and membrane permeability ( 200 nm/s). Both compounds also inhibit both currently circulating oseltamivir-sensitive and-resistant human influenza A viruses (H1N1 and H3N2) with EC50 values ranging from 0.4 to 2.8 mu M and a selectivity index of 100. We also showed for the first time that AM2-S31N channel blockers such as 10e inhibited influenza virus replication at both low and high multiply of infection (10(2)-10(6) pfu/mL) and the inhibition was not cell-type dependent. Overall, these studies have identified two promising lead candidates for further development as antiviral drugs against drug-resistant influenza A viruses.
机译:大多数电流循环流感病毒在其M2基因中携带S31N突变,作为高轮廓的抗病毒靶标呈现AM2-531N。凭借我们持续的兴趣开发AM2-531N通道阻滞剂作为针对奥司唑敏敏敏感和培养的流感病毒的新型抗病毒,我们在此报告了AM2-S31N抑制剂的结构性质关系研究。目标是鉴定具有改善的微粒体稳定性和膜渗透性的铅化合物。发现两个铅化合物,10d和10e具有高小鼠和人肝微粒体稳定性(T-1/2,& 145分钟)和膜渗透率(& 200nm / s)。两种化合物还抑制目前循环奥司他敏敏抗性和抗性的人流感病毒(H1N1和H3N2),EC50值范围为0.4-2.8μm和&gt的选择性指数。 100.我们还表明了AM2-S31N通道阻滞剂(例如10E)的第一次抑制了较低和高乘法的流感病毒复制(10(2)-10(6)PFU / mL),抑制不是细胞 - 依赖于依赖。总体而言,这些研究已经确定了两个有前途的候选人,用于进一步发展作为抗耐药性流感病毒的抗病毒药物。

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