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[原生动物病原体的I型DNA拓扑异构酶作为抗肿瘤药物的潜在靶点]

[Type I DNA topoisomerase from protozoan pathogens as a potential target for anti-tumoral drugs].

作者信息

Reguera Rosa M, Pérez-Pertejo Yolanda, Redondo Carmen M, Díaz-González Rosario, Balaña-Fouce Rafael

机构信息

Departamento de Farmacología y Toxicología (INTOXCAL), Universidad de León, España.

出版信息

Medicina (B Aires). 2007;67(6 Pt 2):747-57.

Abstract

The intensive use of antiparasitic drugs is the main cause of the emergence of multiresistant parasite strains on those regions where these parasites are endemic. The aetiological agents of the so-called tropical diseases viz. malaria, cryptosporidiosis, sleeping sickness, Chagas disease or leishmaniasis, among others, are unicellular protozoan parasites with no immune-prophylactic treatment and where the chemotherapeutical treatment is still under controversy. At present, the chemotherapeutic approach to these diseases is expensive, has side or toxic effects and it does not provide economic profits to the Pharmaceuticals which then have no or scarce enthusiasm in R & D investments in this field. The identification of type I DNA-topoisomerases as promising drug targets is based on the excellent results obtained with camptothecin derivatives in anticancer therapy. The recent finding of significant structural differences between human type I DNA-topoisomerase and their counterparts in trypanosomatids has open a new field in drug discovery, the aim is to find structural insights to be targeted by new drugs. This review is an update of DNA-topoisomerases as potential chemotherapeutic targets against the most important protozoan agents of medical interest.

摘要

在寄生虫流行地区,大量使用抗寄生虫药物是多重耐药寄生虫菌株出现的主要原因。所谓热带疾病的病原体,即疟疾、隐孢子虫病、昏睡病、恰加斯病或利什曼病等,是单细胞原生动物寄生虫,没有免疫预防治疗方法,且化学治疗方法仍存在争议。目前,针对这些疾病的化学治疗方法昂贵,有副作用或毒性,并且不会给制药公司带来经济利润,因此制药公司在该领域的研发投资很少或没有积极性。将I型DNA拓扑异构酶鉴定为有前景的药物靶点是基于喜树碱衍生物在抗癌治疗中取得的优异成果。最近发现人类I型DNA拓扑异构酶与其在锥虫中的对应物之间存在显著结构差异,这为药物发现开辟了一个新领域,目的是找到可供新药靶向的结构见解。这篇综述是关于DNA拓扑异构酶作为针对最重要的具有医学意义的原生动物病原体的潜在化疗靶点的最新情况。

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