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The approved pediatric drug suramin identified as a clinical candidate for the treatment of EV71 infection—suramin inhibits EV71 infection in vitro and in vivo

机译:经批准的儿科药物苏拉明被确定为可治疗EV71感染的临床候选者-苏拉明体外和体内抑制EV71感染

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Enterovirus 71 (EV71) causes severe central nervous system infections, leading to cardiopulmonary complications and death in young children. There is an urgent unmet medical need for new pharmaceutical agents to control EV71 infections. Using a multidisciplinary approach, we found that the approved pediatric antiparasitic drug suramin blocked EV71 infectivity by a novel mechanism of action that involves binding of the naphtalentrisulonic acid group of suramin to the viral capsid. Moreover, we demonstrate that when suramin is used in vivo at doses equivalent to or lower than the highest dose already used in humans, it significantly decreased mortality in mice challenged with a lethal dose of EV71 and peak viral load in adult rhesus monkeys. Thus, suramin inhibits EV71 infection by neutralizing virus particles prior to cell attachment. Consequently, these findings identify suramin as a clinical candidate for further development as a therapeutic or prophylactic treatment for severe EV71 infection.
机译:肠病毒71(EV71)引起严重的中枢神经系统感染,导致心肺并发症并导致幼儿死亡。对于控制EV71感染的新药剂,迫切需要满足医疗需求。使用多学科方法,我们发现批准的儿科抗寄生虫药物苏拉明通过一种新的作用机制阻止了EV71的感染性,该作用机制包括苏拉明的萘四氢苏磺酸酸基团与病毒衣壳的结合。此外,我们证明了当苏拉明在体内以等于或低于人类已经使用的最高剂量的剂量使用时,它显着降低了用致死剂量的EV71攻击的小鼠的死亡率以及成年猕猴的峰值病毒载量。因此,苏拉明通过在附着细胞之前中和病毒颗粒来抑制EV71感染。因此,这些发现确定苏拉明是进一步发展为严重EV71感染的治疗或预防方法的临床候选药物。

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