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烯醇化酶:锥虫寄生虫新陈代谢中的关键因子及可能的毒力因子——作为治疗靶点的应用前景

Enolase: a key player in the metabolism and a probable virulence factor of trypanosomatid parasites-perspectives for its use as a therapeutic target.

作者信息

Avilán Luisana, Gualdrón-López Melisa, Quiñones Wilfredo, González-González Limari, Hannaert Véronique, Michels Paul A M, Concepción Juan-Luis

机构信息

Laboratorio de Fisiología, Facultad de Ciencias, Universidad de los Andes, 5101 Mérida, Venezuela.

出版信息

Enzyme Res. 2011;2011:932549. doi: 10.4061/2011/932549. Epub 2011 Apr 7.

Abstract

Glycolysis and glyconeogenesis play crucial roles in the ATP supply and synthesis of glycoconjugates, important for the viability and virulence, respectively, of the human-pathogenic stages of Trypanosoma brucei, Trypanosoma cruzi, and Leishmania spp. These pathways are, therefore, candidate targets for antiparasite drugs. The glycolytic/gluconeogenic enzyme enolase is generally highly conserved, with similar overall fold and identical catalytic residues in all organisms. Nonetheless, potentially important differences exist between the trypanosomatid and host enzymes, with three unique, reactive residues close to the active site of the former that might be exploited for the development of new drugs. In addition, enolase is found both in the secretome and in association with the surface of Leishmania spp. where it probably functions as plasminogen receptor, playing a role in the parasite's invasiveness and virulence, a function possibly also present in the other trypanosomatids. This location and possible function of enolase offer additional perspectives for both drug discovery and vaccination.

摘要

糖酵解和糖异生在三磷酸腺苷(ATP)供应以及糖缀合物合成过程中发挥着关键作用,这分别对于布氏锥虫、克氏锥虫以及利什曼原虫属人类致病阶段的生存能力和毒力而言至关重要。因此,这些途径是抗寄生虫药物的候选靶点。糖酵解/糖异生酶烯醇化酶通常高度保守,在所有生物体中具有相似的整体折叠结构和相同的催化残基。尽管如此,锥虫类生物与宿主的酶之间可能存在重要差异,前者的活性位点附近有三个独特的反应性残基,可用于开发新药。此外,烯醇化酶在利什曼原虫属的分泌组中以及与该属的表面相关联处均有发现,在那里它可能作为纤溶酶原受体发挥作用,在寄生虫的侵袭性和毒力方面发挥作用,其他锥虫类生物可能也具有此功能。烯醇化酶的这种定位和可能的功能为药物研发和疫苗接种提供了额外的视角。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/703e/3092696/2906cd2a2a9b/ER2011-932549.001.jpg

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