抗疟药物甲氟喹与膜磷脂结合。
The antimalarial drug mefloquine binds to membrane phospholipids.
作者信息
Chevli R, Fitch C D
出版信息
Antimicrob Agents Chemother. 1982 Apr;21(4):581-6. doi: 10.1128/AAC.21.4.581.
Abstract
The new antimalarial drug mefloquine bound with high affinity (Kd approximately 3 X 10-7 M) to membrane lipids of normal mouse erythrocytes and of erythrocytes infected either with chloroquine-susceptible or chloroquine-resistant Plasmodium berghei. Approximately 80 nmol of mefloquine was bound per mg of total lipid. Mefloquine also bound to purified phospholipids with high affinity (Kd approximately 3 X 10-7 M). Phosphatidylinositol and phosphatidylserine bound 300 to 400 nmol of mefloquine per mg. Phosphatidylcholine and phosphatidylethanolamine bound approximately 100 nmol of mefloquine per mg. Mefloquine did not bind to hemoglobin with high affinity, but it bound to free ferriprotoporphyrin IX with a Kd of approximately 3 X 10-7 M. In comparison with mefloquine, chloroquine did not bind effectively to purified phospholipids, although it is known to bind with high affinity to free ferriprotoporphyrin IX. Greater binding to phospholipids may account for the superiority of mefloquine in the treatment of chloroquine-resistant malaria.
摘要
新型抗疟药物甲氟喹以高亲和力(解离常数Kd约为3×10⁻⁷M)与正常小鼠红细胞以及感染了氯喹敏感或氯喹耐药伯氏疟原虫的红细胞的膜脂结合。每毫克总脂质结合约80纳摩尔甲氟喹。甲氟喹也以高亲和力(解离常数Kd约为3×10⁻⁷M)与纯化的磷脂结合。每毫克磷脂酰肌醇和磷脂酰丝氨酸结合300至400纳摩尔甲氟喹。每毫克磷脂酰胆碱和磷脂酰乙醇胺结合约100纳摩尔甲氟喹。甲氟喹不以高亲和力与血红蛋白结合,但它与游离的高铁原卟啉IX结合,解离常数Kd约为3×10⁻⁷M。与甲氟喹相比,氯喹不能有效地与纯化的磷脂结合,尽管已知它能与游离的高铁原卟啉IX以高亲和力结合。与磷脂的更强结合可能解释了甲氟喹在治疗氯喹耐药疟疾方面的优势。
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