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Imidazolopiperazines: Lead Optimization of the Second-Generation Antimalarial Agents

  作者 NAGLE ADVAIT; WU TAO; KUHEN KELLI; GAGARING KERSTIN; BORBOA RACHEL; FRANCEK CAROLINE; CHEN ZHONG; PLOUFFE DAVID; LIN XUENA; CALDWELL CHRISTOPHER; EK JARED; SKOLNIK SUZANNE; LIU FENGHUA; WANG JIANLING; CHANG JONATHAN; LI CHUN; LIU BO; HOLLENBECK THOMAS; TUNTLAND TOVE; ISBELL JOHN; CHUAN TIFFANY; ALPER PHILIP B; FISCHLI CHRISTOPH; BRUN RETO; LAKSHMINARAYANA SURESH B; ROTTMANN MATTHIAS; DIAGANA THIERRY T; WINZELER ELIZABETH A; GLYNNE RICHARD; TULLY DAVID C; CHATTERJEE ARNAB K  
  选自 期刊  Journal of Medicinal Chemistry;  卷期  2012年55-9;  页码  4244-4273  
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[摘要]On the basis of the initial success of optimization of a novel series of imidazolopiperazines, a second generation of compounds involving changes in the core piperazine ring was synthesized to improve antimalarial properties. These changes were carried out to further improve the potency and metabolic stability of the compounds by leveraging the outcome of a set of in vitro metabolic identification studies. The optimized 8,8-dimethyl imidazolopiperazine analogues exhibited improved potency, in vitro metabolic stability profile and, as a result, enhanced oral exposure in vivo in mice. The optimized compounds were found to be more efficacious than the current antimalarials in a malaria mouse model. They exhibit moderate oral exposure in rat pharmacokinetic studies to achieve sufficient multiples of the oral exposure at the efficacious dose in toxicology studies.

 
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