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An Advanced System of the Mitochondrial Processing Peptidase and Core Protein Family in Trypanosoma brucei and Multiple Origins of the Core I Subunit in Eukaryotes

机译:布鲁氏锥虫中线粒体加工肽酶和核心蛋白家族的先进系统以及真核生物中核心I亚基的多种来源

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摘要

Mitochondrial processing peptidase (MPP) consists of α and β subunits that catalyze the cleavage of N-terminal mitochondrial-targeting sequences (N-MTSs) and deliver preproteins to the mitochondria. In plants, both MPP subunits are associated with the respiratory complex bc1, which has been proposed to represent an ancestral form. Subsequent duplication of MPP subunits resulted in separate sets of genes encoding soluble MPP in the matrix and core proteins (cp1 and cp2) of the membrane-embedded bc1 complex. As only α-MPP was duplicated in Neurospora, its single β–MPP functions in both MPP and bc1 complexes. Herein, we investigated the MPP/core protein family and N-MTSs in the kinetoplastid Trypanosoma brucei, which is often considered one of the most ancient eukaryotes. Analysis of N-MTSs predicted in 336 mitochondrial proteins showed that trypanosomal N-MTSs were comparable with N-MTSs from other organisms. N-MTS cleavage is mediated by a standard heterodimeric MPP, which is present in the matrix of procyclic and bloodstream trypanosomes, and its expression is essential for the parasite. Distinct Genes encode cp1 and cp2, and in the bloodstream forms the expression of cp1 is downregulated along with the bc1 complex. Phylogenetic analysis revealed that all eukaryotic lineages include members with a Neurospora-type MPP/core protein family, whereas cp1 evolved independently in metazoans, some fungi and kinetoplastids. Evolution of cp1 allowed the independent regulation of respiration and protein import, which is essential for the procyclic and bloodstream forms of T. brucei. These results indicate that T. brucei possesses a highly derived MPP/core protein family that likely evolved in response to its complex life cycle and does not appear to have an ancient character proposed earlier for this eukaryote.
机译:线粒体加工肽酶(MPP)由α和β亚基组成,可催化N末端线粒体靶向序列(N-MTS)的裂解并将前蛋白传递至线粒体。在植物中,两个MPP亚基都与呼吸复合体bc1相关,后者已被提出代表祖先形式。随后的MPP亚基重复产生了单独的一组基因,这些基因在膜嵌入的bc1复合体的基质和核心蛋白(cp1和cp2)中编码可溶性MPP。由于Neurospora中仅复制了α-MPP,因此其单个β-MPP在MPP和bc1复合物中均起作用。在本文中,我们研究了常被认为是最古老的真核生物之一的运动型布鲁氏锥虫中的MPP /核心蛋白家族和N-MTS。对336个线粒体蛋白中预测的N-MTS的分析表明,锥虫N-MTS与其他生物体的N-MTS相当。 N-MTS裂解是由标准异源二聚体MPP介导的,MPP存在于前环和血流锥虫的基质中,其表达对于寄生虫至关重要。不同的基因编码cp1和cp2,并且在血液中cp1的表达与bc1复合体一起被下调。系统发育分析表明,所有真核细胞系均包含具有神经孢子型MPP /核心蛋白家族的成员,而cp1在后生动物,某些真菌和运动质体中独立进化。 cp1的进化可以独立调节呼吸和蛋白质的导入,这对于布鲁氏锥虫的前循环和血液形式至关重要。这些结果表明布鲁氏杆菌具有高度衍生的MPP /核心蛋白家族,该家族可能响应其复杂的生命周期而进化,并且似乎没有该真核生物先前提出的古老特征。

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