抗疟药咯萘啶对血红素的靶向作用。
Targeting of hematin by the antimalarial pyronaridine.
作者信息
Auparakkitanon Saranya, Chapoomram Soebsakul, Kuaha Kannika, Chirachariyavej Thamrong, Wilairat Prapon
机构信息
Division of Toxicology, Department of Pathology, Faculty of Medicine, Ramathibodi Hospital, Bangkok, Thailand.
出版信息
Antimicrob Agents Chemother. 2006 Jun;50(6):2197-200. doi: 10.1128/AAC.00119-06.
Abstract
Pyronaridine, 2-methoxy-7-chloro-10[3',5'-bis(pyrrolidinyl-1-methyl-)4'hydroxyphenyl]aminobenzyl-(b)-1,5-naphthyridine, a new Mannich base schizontocide originally developed in China and structurally related to the aminoacridine drug quinacrine, is currently undergoing clinical testing. We now show that pyronaridine targets hematin, as demonstrated by its ability to inhibit in vitro beta-hematin formation (at a concentration equal to that of chloroquine), to form a complex with hematin with a stoichiometry of 1:2, to enhance hematin-induced red blood cell lysis (but at 1/100 of the chloroquine concentration), and to inhibit glutathione-dependent degradation of hematin. Our observations that pyronaridine exerted this mechanism of action in situ, based on growth studies of Plasmodium falciparum K1 in culture showing antagonism of pyronaridine in combination with antimalarials (chloroquine, mefloquine, and quinine) that inhibit beta-hematin formation, were equivocal.
摘要
咯萘啶,2-甲氧基-7-氯-10[3',5'-双(吡咯烷基-1-甲基)-4'-羟基苯基]氨基苄基-(β)-1,5-萘啶,一种最初在中国研发的新型曼尼希碱类裂殖体杀灭剂,其结构与氨基吖啶药物奎纳克林相关,目前正在进行临床试验。我们现在表明,咯萘啶靶向血红素,这表现为它能够抑制体外β-血红素的形成(浓度与氯喹相当),与血红素形成化学计量比为1:2的复合物,增强血红素诱导的红细胞裂解(但浓度为氯喹的1/100),并抑制血红素的谷胱甘肽依赖性降解。基于恶性疟原虫K1在培养物中的生长研究,我们观察到咯萘啶在原位发挥这种作用机制,该研究显示咯萘啶与抑制β-血红素形成的抗疟药(氯喹、甲氟喹和奎宁)联合使用时具有拮抗作用,但这些观察结果并不明确。
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