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锥虫复制前机制:一个老问题的潜在新靶点。

Trypanosome prereplication machinery: a potential new target for an old problem.

作者信息

Calderano Simone Guedes, de Melo Godoy Patricia Diogo, da Cunha Julia Pinheiro Chagas, Elias Maria Carolina

机构信息

Laboratório Especial de Toxinologia Aplicada (LETA) Center for Applied Toxinology (CAT/CEPID), Instituto Butantan, Avenida Vital Brasil 1500, 05503-000 São Paulo, SP, Brazil.

出版信息

Enzyme Res. 2011;2011:518258. doi: 10.4061/2011/518258. Epub 2011 May 25.

Abstract

Approximately ten million people suffer from Chagas disease worldwide, caused by Trypanosoma cruzi, with the disease burden predominately focused in Latin America. Sleeping sickness is another serious health problem, caused by Trypanosoma brucei, especially in sub-Saharan countries. Unfortunately, the drugs currently available to treat these diseases have toxic effects and are not effective against all disease phases or parasite strains. Therefore, there is a clear need for the development of novel drugs and drug targets to treat these diseases. We propose the trypanosome prereplication machinery component, Orc1/Cdc6, as a potential target for drug development. In trypanosomes, Orc1/Cdc6 is involved in nuclear DNA replication, and, despite its involvement in such a conserved process, Orc1/Cdc6 is distinct from mammalian Orc1 and Cdc6 proteins. Moreover, RNAi-mediated silencing of trypanosome Orc1/Cdc6 expression in T. brucei decreased cell survival, indicating that Orc1/Cdc6 is critical for trypanosome survival.

摘要

全球约有1000万人患有恰加斯病,该病由克氏锥虫引起,疾病负担主要集中在拉丁美洲。昏睡病是另一个严重的健康问题,由布氏锥虫引起,特别是在撒哈拉以南国家。不幸的是,目前可用于治疗这些疾病的药物具有毒性作用,并且对所有疾病阶段或寄生虫菌株均无效。因此,显然需要开发新型药物和药物靶点来治疗这些疾病。我们提出锥虫复制前机制组件Orc1/Cdc6作为药物开发的潜在靶点。在锥虫中,Orc1/Cdc6参与核DNA复制,并且尽管其参与如此保守的过程,但Orc1/Cdc6与哺乳动物的Orc1和Cdc6蛋白不同。此外,RNAi介导的布氏锥虫中锥虫Orc1/Cdc6表达的沉默降低了细胞存活率,表明Orc1/Cdc6对锥虫存活至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/60b3/3112515/72131dde0b74/ER2011-518258.001.jpg

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