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Δ1-吡咯啉-5-羧酸脱氢酶的作用支持克氏锥虫的线粒体代谢和宿主细胞入侵。

Role of Δ1-pyrroline-5-carboxylate dehydrogenase supports mitochondrial metabolism and host-cell invasion of Trypanosoma cruzi.

作者信息

Mantilla Brian S, Paes Lisvane S, Pral Elizabeth M F, Martil Daiana E, Thiemann Otavio H, Fernández-Silva Patricio, Bastos Erick L, Silber Ariel M

机构信息

From the Instituto de Ciências Biomédicas, Departamento de Parasitologia, Universidade de São Paulo, 05508-000 São Paulo, Brazil.

the Laboratório de Biologia Estrutural, Instituto de Física de São Carlos, and.

出版信息

J Biol Chem. 2015 Mar 20;290(12):7767-90. doi: 10.1074/jbc.M114.574525. Epub 2015 Jan 26.

Abstract

Proline is crucial for energizing critical events throughout the life cycle of Trypanosoma cruzi, the etiological agent of Chagas disease. The proline breakdown pathway consists of two oxidation steps, both of which produce reducing equivalents as follows: the conversion of proline to Δ(1)-pyrroline-5-carboxylate (P5C), and the subsequent conversion of P5C to glutamate. We have identified and characterized the Δ(1)-pyrroline-5-carboxylate dehydrogenase from T. cruzi (TcP5CDH) and report here on how this enzyme contributes to a central metabolic pathway in this parasite. Size-exclusion chromatography, two-dimensional gel electrophoresis, and small angle x-ray scattering analysis of TcP5CDH revealed an oligomeric state composed of two subunits of six protomers. TcP5CDH was found to complement a yeast strain deficient in PUT2 activity, confirming the enzyme's functional role; and the biochemical parameters (Km, kcat, and kcat/Km) of the recombinant TcP5CDH were determined, exhibiting values comparable with those from T. cruzi lysates. In addition, TcP5CDH exhibited mitochondrial staining during the main stages of the T. cruzi life cycle. mRNA and enzymatic activity levels indicated the up-regulation (6-fold change) of TcP5CDH during the infective stages of the parasite. The participation of P5C as an energy source was also demonstrated. Overall, we propose that this enzymatic step is crucial for the viability of both replicative and infective forms of T. cruzi.

摘要

脯氨酸对于恰加斯病的病原体克氏锥虫整个生命周期中的关键活动供能至关重要。脯氨酸分解途径包括两个氧化步骤,两者都会产生还原当量,具体如下:脯氨酸转化为Δ(1)-吡咯啉-5-羧酸(P5C),随后P5C转化为谷氨酸。我们已经鉴定并表征了来自克氏锥虫的Δ(1)-吡咯啉-5-羧酸脱氢酶(TcP5CDH),并在此报告该酶如何参与这种寄生虫的中心代谢途径。对TcP5CDH进行的尺寸排阻色谱、二维凝胶电泳和小角X射线散射分析显示,其寡聚状态由六个原体的两个亚基组成。发现TcP5CDH可补充PUT2活性缺陷的酵母菌株,证实了该酶的功能作用;并测定了重组TcP5CDH的生化参数(Km、kcat和kcat/Km),其值与克氏锥虫裂解物的值相当。此外,在克氏锥虫生命周期的主要阶段,TcP5CDH表现出线粒体染色。mRNA和酶活性水平表明,在寄生虫的感染阶段,TcP5CDH上调(6倍变化)。还证明了P5C作为能量来源的参与。总体而言,我们认为这一酶促步骤对于克氏锥虫复制型和感染型的生存能力至关重要。

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