Inhibition of mitosomal alternative oxidase causes lifecycle arrest of early-stage Trachipleistophora hominis meronts during intracellular infection of mammalian cells

Mitosomes are highly reduced forms of mitochondria which have lost two of the 'defining' features of the canonical organelle, the mitochondrial genome, and the capacity to generate energy in the form of ATP. Mitosomes are found in anaerobic protists and obligate parasites and, in most of t...

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Veröffentlicht in:	PLoS pathogens 2022-12, Vol.18 (12), p.e1011024
Hauptverfasser:	Sendra, Kacper M, Watson, Andrew K, Kozhevnikova, Ekaterina, Moore, Anthony L, Embley, T Martin, Hirt, Robert P
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Sprache:	eng
Schlagworte:	Albendazole Alternative oxidase Animals Antibodies Antiinfectives and antibacterials Antimicrobial agents Biology Biology and Life Sciences Biosynthesis Cell interaction Cell lines Chemical compounds Clusters Cofactors Dehydrogenases Diseases Enzymes Fungal Proteins - metabolism Genomes Glycerol Host-parasite relationships Humans Infections Iron Life cycle analysis Life Cycle Stages Life cycles Life cycles (Biology) Localization Mammalian cells Mammals Medicine and Health Sciences Microsporidia Mitochondria Oxidase Oxidases Oxidoreductases - genetics Parasites Parasitological research Pharmacology Physiological aspects Proteins Research and Analysis Methods Respiration Spores Sulfur
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description	Mitosomes are highly reduced forms of mitochondria which have lost two of the 'defining' features of the canonical organelle, the mitochondrial genome, and the capacity to generate energy in the form of ATP. Mitosomes are found in anaerobic protists and obligate parasites and, in most of the studied organisms, have a conserved function in the biosynthesis of iron-sulfur clusters (ISC) that are indispensable cofactors of many essential proteins. The genomes of some mitosome-bearing human pathogenic Microsporidia encode homologues of an alternative oxidase (AOX). This mitochondrial terminal respiratory oxidase is absent from the human host, and hence is a potential target for the development of new antimicrobial agents. Here we present experimental evidence for the mitosomal localization of AOX in the microsporidian Trachipleistophora hominis and demonstrate that it has an important role during the parasite's life cycle progression. Using a recently published methodology for synchronising T. hominis infection of mammalian cell lines, we demonstrated specific inhibition of T. hominis early meront growth and replication by an AOX inhibitor colletochlorin B. Treatment of T. hominis-infected host cells with the drug also inhibited re-infection by newly formed dispersive spores. Addition of the drug during the later stages of the parasite life cycle, when our methods suggest that AOX is not actively produced and T. hominis mitosomes are mainly active in Fe/S cluster biosynthesis, had no inhibitory effects on the parasites. Control experiments with the AOX-deficient microsporidian species Encephalitozoon cuniculi, further demonstrated the specificity of inhibition by the drug. Using the same methodology, we demonstrate effects of two clinically used anti-microsporidian drugs albendazole and fumagillin on the cell biology and life cycle progression of T. hominis infecting mammalian host cells. In summary, our results reveal that T. hominis mitosomes have an active role to play in the progression of the parasite life cycle as well as an important role in the biosynthesis of essential Fe/S clusters. Our work also demonstrates that T. hominis is a useful model for testing the efficacy of therapeutic agents and for studying the physiology and cell biology of microsporidian parasites growing inside infected mammalian cells.
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Mitosomes are found in anaerobic protists and obligate parasites and, in most of the studied organisms, have a conserved function in the biosynthesis of iron-sulfur clusters (ISC) that are indispensable cofactors of many essential proteins. The genomes of some mitosome-bearing human pathogenic Microsporidia encode homologues of an alternative oxidase (AOX). This mitochondrial terminal respiratory oxidase is absent from the human host, and hence is a potential target for the development of new antimicrobial agents. Here we present experimental evidence for the mitosomal localization of AOX in the microsporidian Trachipleistophora hominis and demonstrate that it has an important role during the parasite's life cycle progression. Using a recently published methodology for synchronising T. hominis infection of mammalian cell lines, we demonstrated specific inhibition of T. hominis early meront growth and replication by an AOX inhibitor colletochlorin B. Treatment of T. hominis-infected host cells with the drug also inhibited re-infection by newly formed dispersive spores. Addition of the drug during the later stages of the parasite life cycle, when our methods suggest that AOX is not actively produced and T. hominis mitosomes are mainly active in Fe/S cluster biosynthesis, had no inhibitory effects on the parasites. Control experiments with the AOX-deficient microsporidian species Encephalitozoon cuniculi, further demonstrated the specificity of inhibition by the drug. Using the same methodology, we demonstrate effects of two clinically used anti-microsporidian drugs albendazole and fumagillin on the cell biology and life cycle progression of T. hominis infecting mammalian host cells. In summary, our results reveal that T. hominis mitosomes have an active role to play in the progression of the parasite life cycle as well as an important role in the biosynthesis of essential Fe/S clusters. 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This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.</rights><rights>COPYRIGHT 2022 Public Library of Science</rights><rights>2022 Sendra et al. This is an open access article distributed under the terms of the Creative Commons Attribution License: http://creativecommons.org/licenses/by/4.0/ (the “License”), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. 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Treatment of T. hominis-infected host cells with the drug also inhibited re-infection by newly formed dispersive spores. Addition of the drug during the later stages of the parasite life cycle, when our methods suggest that AOX is not actively produced and T. hominis mitosomes are mainly active in Fe/S cluster biosynthesis, had no inhibitory effects on the parasites. Control experiments with the AOX-deficient microsporidian species Encephalitozoon cuniculi, further demonstrated the specificity of inhibition by the drug. Using the same methodology, we demonstrate effects of two clinically used anti-microsporidian drugs albendazole and fumagillin on the cell biology and life cycle progression of T. hominis infecting mammalian host cells. In summary, our results reveal that T. hominis mitosomes have an active role to play in the progression of the parasite life cycle as well as an important role in the biosynthesis of essential Fe/S clusters. Our work also demonstrates that T. hominis is a useful model for testing the efficacy of therapeutic agents and for studying the physiology and cell biology of microsporidian parasites growing inside infected mammalian cells.</description><subject>Albendazole</subject><subject>Alternative oxidase</subject><subject>Animals</subject><subject>Antibodies</subject><subject>Antiinfectives and antibacterials</subject><subject>Antimicrobial agents</subject><subject>Biology</subject><subject>Biology and Life Sciences</subject><subject>Biosynthesis</subject><subject>Cell interaction</subject><subject>Cell lines</subject><subject>Chemical compounds</subject><subject>Clusters</subject><subject>Cofactors</subject><subject>Dehydrogenases</subject><subject>Diseases</subject><subject>Enzymes</subject><subject>Fungal Proteins - metabolism</subject><subject>Genomes</subject><subject>Glycerol</subject><subject>Host-parasite relationships</subject><subject>Humans</subject><subject>Infections</subject><subject>Iron</subject><subject>Life cycle analysis</subject><subject>Life Cycle Stages</subject><subject>Life cycles</subject><subject>Life cycles (Biology)</subject><subject>Localization</subject><subject>Mammalian cells</subject><subject>Mammals</subject><subject>Medicine and Health Sciences</subject><subject>Microsporidia</subject><subject>Mitochondria</subject><subject>Oxidase</subject><subject>Oxidases</subject><subject>Oxidoreductases - 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Mitosomes are found in anaerobic protists and obligate parasites and, in most of the studied organisms, have a conserved function in the biosynthesis of iron-sulfur clusters (ISC) that are indispensable cofactors of many essential proteins. The genomes of some mitosome-bearing human pathogenic Microsporidia encode homologues of an alternative oxidase (AOX). This mitochondrial terminal respiratory oxidase is absent from the human host, and hence is a potential target for the development of new antimicrobial agents. Here we present experimental evidence for the mitosomal localization of AOX in the microsporidian Trachipleistophora hominis and demonstrate that it has an important role during the parasite's life cycle progression. Using a recently published methodology for synchronising T. hominis infection of mammalian cell lines, we demonstrated specific inhibition of T. hominis early meront growth and replication by an AOX inhibitor colletochlorin B. 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subjects	Albendazole Alternative oxidase Animals Antibodies Antiinfectives and antibacterials Antimicrobial agents Biology Biology and Life Sciences Biosynthesis Cell interaction Cell lines Chemical compounds Clusters Cofactors Dehydrogenases Diseases Enzymes Fungal Proteins - metabolism Genomes Glycerol Host-parasite relationships Humans Infections Iron Life cycle analysis Life Cycle Stages Life cycles Life cycles (Biology) Localization Mammalian cells Mammals Medicine and Health Sciences Microsporidia Mitochondria Oxidase Oxidases Oxidoreductases - genetics Parasites Parasitological research Pharmacology Physiological aspects Proteins Research and Analysis Methods Respiration Spores Sulfur
title	Inhibition of mitosomal alternative oxidase causes lifecycle arrest of early-stage Trachipleistophora hominis meronts during intracellular infection of mammalian cells
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