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Characterization of Evolutionarily Conserved Trypanosoma cruzi NatC and NatA-N-Terminal Acetyltransferase Complexes

机译:进化上保守的克氏锥虫NatC和NatA-N末端乙酰转移酶复合物的表征。

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摘要

Protein N-terminal acetylation is a co- and posttranslational modification, conserved among eukaryotes. It determines the functional fate of many proteins including their stability, complex formation, and subcellular localization. N-terminal acetyltransferases (NATs) transfer an acetyl group to the N-termini of proteins, and the major NATs in yeast and humans are NatA, NatB, and NatC. In this study, we characterized the Trypanosoma cruzi (T. cruzi) NatC and NatA protein complexes, each consisting of one catalytic subunit and predicted auxiliary subunits. The proteins were found to be expressed in the three main life cycle stages of the parasite, formed stable complexes in vivo, and partially cosedimented with the ribosome in agreement with a cotranslational function. An in vitro acetylation assay clearly demonstrated that the acetylated substrates of the NatC catalytic subunit from T. cruzi were similar to those of yeast and human NatC, suggesting evolutionary conservation of function. An RNAi knockdown of the Trypanosoma brucei (T. brucei) NatC catalytic subunit indicated that reduced NatC-mediated N-terminal acetylation of target proteins reduces parasite growth.
机译:蛋白N-末端乙酰化是真核生物中保守的共翻译和翻译后修饰。它决定了许多蛋白质的功能命运,包括它们的稳定性,复合物的形成和亚细胞定位。 N末端乙酰基转移酶(NAT)将乙酰基转移到蛋白质的N末端,酵母和人类中的主要NAT是NatA,NatB和NatC。在这项研究中,我们表征了锥虫(T. cruzi)NatC和NatA蛋白复合物,每种复合物均由一个催化亚基和预测的辅助亚基组成。发现该蛋白质在该寄生虫的三个主要生命周期阶段中表达,在体内形成稳定的复合物,并与核糖体部分共沉淀,并具有共翻译功能。体外乙酰化分析清楚地表明,来自克鲁维酵母的NatC催化亚基的乙酰化底物与酵母和人NatC的底物相似,表明功能的进化保守性。布鲁氏锥虫(T. brucei)NatC催化亚基的RNAi敲低表明目标蛋白的NatC介导的N末端乙酰化程度降低会降低寄生虫的生长。

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