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首页> 外文期刊>Scientific reports. >Griseofulvin impairs intraerythrocytic growth of Plasmodium falciparum through ferrochelatase inhibition but lacks activity in an experimental human infection study
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Griseofulvin impairs intraerythrocytic growth of Plasmodium falciparum through ferrochelatase inhibition but lacks activity in an experimental human infection study

机译:Griseofulvin通过铁素酸酶抑制损害疟原虫的嗜疟原虫细胞植物生长,但缺乏在实验性人体感染研究中的活性

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Griseofulvin, an orally active antifungal drug used to treat dermatophyte infections, has a secondary effect of inducing cytochrome P450-mediated production of N-methyl protoporphyrin IX (N-MPP). N-MPP is a potent competitive inhibitor of the heme biosynthetic-enzyme ferrochelatase, and inhibits the growth of cultured erythrocyte stage Plasmodium falciparum. Novel drugs against Plasmodium are needed to achieve malaria elimination. Thus, we investigated whether griseofulvin shows anti-plasmodial activity. We observed that the intraerythrocytic growth of P. falciparum is inhibited in red blood cells pretreated with griseofulvin in vitro. Treatment with 100?μM griseofulvin was sufficient to prevent parasite growth and induce the production of N-MPP. Inclusion of the ferrochelatase substrate PPIX blocked the inhibitory activity of griseofulvin, suggesting that griseofulvin exerts its activity through the N-MPP-dependent inhibition of ferrochelatase. In an ex-vivo study, red blood cells from griseofulvin-treated subjects were refractory to the growth of cultured P. falciparum. However, in a clinical trial griseofulvin failed to show either therapeutic or prophylactic effect in subjects infected with blood stage P. falciparum. Although the development of griseofulvin as an antimalarial is not warranted, it represents a novel inhibitor of P. falciparum growth and acts via the N-MPP-dependent inhibition of ferrochelatase.
机译:Griseofulvin是一种用于治疗Dermatophyte感染的口服活性抗真菌药物,具有诱导细胞色素P450介导的N-甲基原子卟啉IX(N-MPP)的二次效果。 N-MPP是血红素生物合成酶铁切酶的有效竞争性抑制剂,抑制培养的红细胞阶段疟原虫的生长。需要对疟原虫进行新药来实现疟疾消除。因此,我们研究了Griseofulvin是否显示出抗疟原虫活性。我们观察到,在体外用Griseofulvin预处理的红细胞抑制了P. falciparum的肝癌的生长。用100μM1μmGriseofulvin处理足以防止寄生虫生长并诱导N-MPP的产生。包含铁素酶底物ppix阻断了Griseofulvin的抑制活性,表明Griseofulvin通过N-MPP依赖性抑制铁素酶施加活性。在前体内研究中,来自Griseofulvin治疗的受试者的红细胞对培养的P. falciparum的生长是难治的。然而,在临床试验中,Griseofulvin未能显示在感染的受试者中展示治疗或预防效果P. Falciparum。虽然不保证Griseofulvin作为抗疟疾的发展,但它代表了一种新的P. falciparum生长的抑制剂,并通过N-MPP依赖性抑制铁素酸酶。

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