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啮齿动物疟疾的化学疗法,三十八。三种新型抗疟药(WR 194,965、WR 228,258和WR 225,448)对啮齿动物和人类疟原虫(伯氏疟原虫和恶性疟原虫)活性的研究。

The chemotherapy of rodent malaria, XXXVIII. Studies on the activity of three new antimalarials (WR 194,965, WR 228,258 and WR 225,448) against rodent and human malaria parasites (Plasmodium berghei and P. falciparum).

作者信息

Peters W, Irare S G, Ellis D S, Warhurst D C, Robinson B L

出版信息

Ann Trop Med Parasitol. 1984 Dec;78(6):567-79.

PMID:6398032
Abstract

In addition to their blood schizontocidal action on Plasmodium berghei in vivo, two Mannich bases WR 194,965 and 228,258 are also active against chloroquine-sensitive and chloroquine-resistant lines of P. falciparum in vitro. The response of the lines to each drug differs but shows no correlation in either case with response to chloroquine. The 8-aminoquinoline WR 225,448 is also active against P. falciparum in vitro but at much higher concentrations than the Mannich bases. Application of the 'chloroquine-induced pigment clumping (CIPC) test' and the study of ultrastructural changes induced in P. berghei in drug-treated mice indicate that WR 194,965 has a mode of action somewhat resembling that of quinine. WR 228,258 in vitro shows a chloroquine-like effect, but not in vivo, suggesting that its mode of action in vivo is different from that of chloroquine. WR 225,448 has no action in the CIPC in vitro and affects primarily mitochondria of the parasites in vivo. It probably acts through a metabolite. Both pre-erythrocytic and erythrocytic stages of rodent malaria parasites are affected by WR 225,448.

摘要

除了在体内对伯氏疟原虫具有血内裂殖体杀灭作用外,两种曼尼希碱WR 194,965和228,258在体外对氯喹敏感和氯喹耐药的恶性疟原虫株也具有活性。各株对每种药物的反应不同,但在这两种情况下与对氯喹的反应均无相关性。8-氨基喹啉WR 225,448在体外对恶性疟原虫也具有活性,但浓度远高于曼尼希碱。应用“氯喹诱导色素凝聚(CIPC)试验”以及对药物处理小鼠体内伯氏疟原虫诱导的超微结构变化的研究表明,WR 194,965的作用方式 somewhat resembling that of quinine(此处原文有误,疑为“somewhat resembling that of chloroquine”,意为“有点类似于氯喹的作用方式”)。WR 228,258在体外显示出类似氯喹的作用,但在体内并非如此,这表明其在体内的作用方式与氯喹不同。WR 225,448在体外CIPC试验中无作用,在体内主要影响疟原虫的线粒体。它可能通过一种代谢产物起作用。啮齿动物疟原虫的前红细胞期和红细胞期均受WR 225,448影响。

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