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一种对非洲锥虫晚期θ结构解析至关重要的线粒体拓扑异构酶IA。

A mitochondrial topoisomerase IA essential for late theta structure resolution in African trypanosomes.

作者信息

Scocca Jane R, Shapiro Theresa A

机构信息

Division of Clinical Pharmacology, Department of Medicine and of Pharmacology, The Johns Hopkins University School of Medicine, Baltimore, MD, USA.

出版信息

Mol Microbiol. 2008 Feb;67(4):820-9. doi: 10.1111/j.1365-2958.2007.06087.x. Epub 2007 Dec 19.

Abstract

Trypanosomes and Leishmania, protozoans that cause major human diseases, have a topologically intricate mitochondrial DNA (kinetoplast or kDNA) in the form of a network of thousands of interlocked circles. This unusual system provides a useful reporter for studying topoisomerase functions in vivo. We now find that these organisms have three type IA topoisomerases, one of which is phylogenetically distinctive and which we designate topoisomerase IA(mt). In Trypanosoma brucei topoisomerase IA(mt) immunolocalizes within the mitochondrion close to the kDNA disk in patterns that vary with the cell cycle. When expression of TOPIA(mt) is silenced by RNAi there is a striking accumulation of kDNA late theta structure replication intermediates, with subsequent loss of kDNA networks and halt in cell growth. This essential enzyme provides clear molecular evidence for the obligatory role of a type IA enzyme in the resolution of late theta structures in vivo. With no close orthologue in humans it also offers a target for the rational development of selectively toxic new antiprotozoal therapies.

摘要

锥虫和利什曼原虫是导致人类重大疾病的原生动物,它们具有拓扑结构复杂的线粒体DNA(动质体或kDNA),呈由数千个互锁环组成的网络形式。这个不同寻常的系统为研究拓扑异构酶在体内的功能提供了一个有用的报告分子。我们现在发现这些生物体有三种IA型拓扑异构酶,其中一种在系统发育上具有独特性,我们将其命名为拓扑异构酶IA(mt)。在布氏锥虫中,拓扑异构酶IA(mt)通过免疫定位在线粒体内靠近kDNA盘的位置,其模式随细胞周期而变化。当通过RNA干扰使TOPIA(mt)的表达沉默时,kDNA晚期θ结构复制中间体显著积累,随后kDNA网络丢失,细胞生长停止。这种必需的酶为IA型酶在体内解决晚期θ结构中的 obligatory 作用提供了明确的分子证据。由于在人类中没有密切的直系同源物,它也为合理开发选择性毒性新抗寄生虫疗法提供了一个靶点。 (注:“obligatory”此处结合语境推测可能是“必不可少的”之类意思,但不确定准确意思,原文可能有误,正常应为“obligatory”的正确形式相关词汇。)

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