Reductive Evolution of the Mitochondrial Processing Peptidases of the Unicellular Parasites Trichomonas vaginalis and Giardia intestinalis
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| Authors: | Ond?ej ?míd Anna Matu?ková Simon R Harris Tomá? Ku?era Marián Novotny Lenka Horváthová Ivan Hrdy Eva Kutějová Robert P Hirt T Martin Embley Ji?í Janata Jan Tachezy |
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| Institution: | 1. Department of Parasitology, Faculty of Science, Charles University in Prague, Prague, Czech Republic.; 2. Institute of Microbiology, Academy of Sciences of the Czech Republic, Prague, Czech Republic.; 3. Institute for Cell and Molecular Biosciences, Newcastle University, Newcastle upon Tyne, United Kingdom.; 4. Institute of Molecular Biology, Slovak Academy of Sciences, Bratislava, Slovak Republic.;Washington University School of Medicine, United States of America |
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| Abstract: | Mitochondrial processing peptidases are heterodimeric enzymes (α/βMPP) that play an essential role in mitochondrial biogenesis by recognizing and cleaving the targeting presequences of nuclear-encoded mitochondrial proteins. The two subunits are paralogues that probably evolved by duplication of a gene for a monomeric metallopeptidase from the endosymbiotic ancestor of mitochondria. Here, we characterize the MPP-like proteins from two important human parasites that contain highly reduced versions of mitochondria, the mitosomes of Giardia intestinalis and the hydrogenosomes of Trichomonas vaginalis. Our biochemical characterization of recombinant proteins showed that, contrary to a recent report, the Trichomonas processing peptidase functions efficiently as an α/β heterodimer. By contrast, and so far uniquely among eukaryotes, the Giardia processing peptidase functions as a monomer comprising a single βMPP-like catalytic subunit. The structure and surface charge distribution of the Giardia processing peptidase predicted from a 3-D protein model appear to have co-evolved with the properties of Giardia mitosomal targeting sequences, which, unlike classic mitochondrial targeting signals, are typically short and impoverished in positively charged residues. The majority of hydrogenosomal presequences resemble those of mitosomes, but longer, positively charged mitochondrial-type presequences were also identified, consistent with the retention of the Trichomonas αMPP-like subunit. Our computational and experimental/functional analyses reveal that the divergent processing peptidases of Giardia mitosomes and Trichomonas hydrogenosomes evolved from the same ancestral heterodimeric α/βMPP metallopeptidase as did the classic mitochondrial enzyme. The unique monomeric structure of the Giardia enzyme, and the co-evolving properties of the Giardia enzyme and substrate, provide a compelling example of the power of reductive evolution to shape parasite biology. |
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