Cure with cisplatin (II) or murine malaria infection and in vitro inhibition of a chloroquine-resistant Plasmodium falciparum isolate.

L Nair, V K Bhasin
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引用次数: 17

Abstract

Antiplasmodium properties of cisplatin [cis-platinum (II) diamine dichloride], a neoplastic drug, have been assessed in in vivo and in vitro model systems of malarial parasite. A well-tolerated dose of 6 mg/kg body weight of the compound cured the mice infected with Plasmodium berghei and the amount of cisplatin required for in vitro inhibition (IC50) of a chloroquine-resistant Plasmodium falciparum isolate was smaller than either chloroquine or quinine. The minimum inhibitory concentration (MIC) needed to prevent the in vitro multiplication of asexual blood parasites was 30 ng/ml. Late ring and trophozoite stages of the erythrocytic cycle were the most susceptible, whereas schizont and early ring stages were the least sensitive to the toxic effect of cisplatin. Multiple smaller doses were more effective in curing malaria in mice than a single large dose. In a few of the mice treated with a single intraperitoneal large dose of 6 mg/kg body weight, there was a delay in appearance of parasitemia but most of them recovered completely but slowly. This compound exerts its toxicity mainly by randomly damaging and cross-linking DNA strands as shown by Southern hybridization with a synthetic oligonucleotide probe, which is a repeat sequence in the falciparum genome. The report clearly demonstrates the antimalarial potentials of this compound and suggests a closer evaluation of this and other related compounds, specially in combination with antimalarial drugs to probe their synergistic properties.

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治疗顺铂(II)或小鼠疟疾感染和体外抑制氯喹耐药恶性疟原虫分离物。
肿瘤药物顺铂[顺铂(II)二胺二氯化]的抗疟原虫特性已在体内和体外疟疾寄生虫模型系统中进行了评估。6 mg/kg体重的良好耐受剂量的化合物治愈了感染伯氏疟原虫的小鼠,并且对氯喹耐药恶性疟原虫分离物的体外抑制(IC50)所需的顺铂量小于氯喹或奎宁。抑制无性血寄生虫体外增殖所需的最低抑菌浓度为30 ng/ml。晚期环和滋养体阶段对顺铂的毒性作用最敏感,而分裂体和早期环对顺铂的毒性作用最不敏感。在治疗小鼠疟疾方面,多次小剂量比单次大剂量更有效。少数小鼠单次腹腔注射大剂量6 mg/kg体重,出现寄生虫病有延迟,但大多数完全恢复,但恢复缓慢。该化合物主要通过随机破坏和交联DNA链来发挥其毒性,如与合成寡核苷酸探针的南方杂交所示,这是恶性疟原虫基因组中的重复序列。该报告清楚地证明了该化合物的抗疟疾潜力,并建议对该化合物和其他相关化合物进行更密切的评估,特别是与抗疟疾药物联合使用以探索其协同特性。
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