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New Bis-thiazolium Analogues as Potential Antimalarial Agents: Design, Synthesis, and Biological Evaluation

  作者 CALDARELLI SERGIO A; EL FANGOUR SIHAM; WEIN SHARON; VAN BA CHRISTOPHE TRAN; PERIGAUD CHRISTIAN; PELLET ALAIN; VIAL HENRI J; PEYROTTES SUZANNE  
  选自 期刊  Journal of Medicinal Chemistry;  卷期  2013年56-2;  页码  496-509  
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[摘要]Bis-thiazolium salts are able to inhibit phosphatidylcholine biosynthesis in Plasmodium and to block parasite proliferation in the low nanomolar range. However, due to their physicochemical properties (i.e., permanent cationic charges, the flexibility, and lipophilic character of the alkyl chain), the oral bioavailability of these compounds is low. New series of bis-thiazolium-based drugs have been designed to overcome this drawback. They feature linker rigidification via the introduction of aromatic rings and/or a decrease in the overall lipophilicity through the introduction of heteroatoms. On the basis of the structure-activity relationships, a few of the promising compounds (9, 10, and 11) were found to exhibit potent antimalarial in vitro and in vivo activities (EC50 < 10 nM and ED50 ip < 0.7 mg/kg).

 
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