Generation of trans-mitochondrial mice carrying homoplasmic mtDNAs with a missense mutation in a structural gene using ES cells

Generation of various kinds of trans-mitochondrial mice, mito-mice, each carrying mtDNAs with a different pathogenic mutation, is required for precise investigation of the pathogenesis of mitochondrial diseases. This study used two respiration-deficient mouse cell lines as donors of mtDNAs with poss...

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Veröffentlicht in:	Human molecular genetics 2006-03, Vol.15 (6), p.871-881
Hauptverfasser:	Kasahara, Atsuko, Ishikawa, Kaori, Yamaoka, Makiko, Ito, Masahito, Watanabe, Naoki, Akimoto, Miho, Sato, Akitsugu, Nakada, Kazuto, Endo, Hitoshi, Suda, Yoko, Aizawa, Shinichi, Hayashi, Jun-Ichi
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Schlagworte:	Animals Biological and medical sciences Cell Line Cell Respiration - genetics Chimera Crosses, Genetic DNA, Mitochondrial - genetics Embryonic Stem Cells - metabolism Embryonic Stem Cells - pathology Embryonic Stem Cells - transplantation Female Fundamental and applied biological sciences. Psychology Genetics of eukaryotes. Biological and molecular evolution Male Mice Mice, Inbred BALB C Mice, Inbred C57BL Mice, Inbred ICR Mice, Nude Mice, Transgenic Mitochondria - genetics Molecular and cellular biology Mutation, Missense Phenotype Point Mutation Rats Rats, Wistar Rattus norvegicus
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container_title	Human molecular genetics
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creator	Kasahara, Atsuko Ishikawa, Kaori Yamaoka, Makiko Ito, Masahito Watanabe, Naoki Akimoto, Miho Sato, Akitsugu Nakada, Kazuto Endo, Hitoshi Suda, Yoko Aizawa, Shinichi Hayashi, Jun-Ichi
description	Generation of various kinds of trans-mitochondrial mice, mito-mice, each carrying mtDNAs with a different pathogenic mutation, is required for precise investigation of the pathogenesis of mitochondrial diseases. This study used two respiration-deficient mouse cell lines as donors of mtDNAs with possible pathogenic mutations. One cell line expressed 45–50% respiratory activity due to mouse mtDNAs with a T6589C missense mutation in the COI gene (T6589C mtDNA) and the other expressed 40% respiratory activity due to rat (Rattus norvegicus) mtDNAs in mouse cells. By cytoplasmic transfer of these mtDNAs to mouse ES cells, we isolated respiration-deficient ES cells. We obtained chimeric mice and generated their F6 progeny carrying mouse T6589C mtDNAs by its female germ line transmission. They were respiration-deficient and thus could be used as models of mitochondrial diseases caused by point mutations in mtDNA structural genes. However, chimeric mice and mito-mice carrying rat mtDNAs were not obtained, suggesting that significant respiration defects or some deficits induced by rat mtDNAs in mouse ES cells prevented their differentiation to generate mice carrying rat mtDNAs.
doi_str_mv	10.1093/hmg/ddl005
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Mol. Genet</addtitle><description>Generation of various kinds of trans-mitochondrial mice, mito-mice, each carrying mtDNAs with a different pathogenic mutation, is required for precise investigation of the pathogenesis of mitochondrial diseases. This study used two respiration-deficient mouse cell lines as donors of mtDNAs with possible pathogenic mutations. One cell line expressed 45–50% respiratory activity due to mouse mtDNAs with a T6589C missense mutation in the COI gene (T6589C mtDNA) and the other expressed 40% respiratory activity due to rat (Rattus norvegicus) mtDNAs in mouse cells. By cytoplasmic transfer of these mtDNAs to mouse ES cells, we isolated respiration-deficient ES cells. We obtained chimeric mice and generated their F6 progeny carrying mouse T6589C mtDNAs by its female germ line transmission. They were respiration-deficient and thus could be used as models of mitochondrial diseases caused by point mutations in mtDNA structural genes. 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Mol. Genet</addtitle><date>2006-03-15</date><risdate>2006</risdate><volume>15</volume><issue>6</issue><spage>871</spage><epage>881</epage><pages>871-881</pages><issn>0964-6906</issn><eissn>1460-2083</eissn><coden>HNGEE5</coden><abstract>Generation of various kinds of trans-mitochondrial mice, mito-mice, each carrying mtDNAs with a different pathogenic mutation, is required for precise investigation of the pathogenesis of mitochondrial diseases. This study used two respiration-deficient mouse cell lines as donors of mtDNAs with possible pathogenic mutations. One cell line expressed 45–50% respiratory activity due to mouse mtDNAs with a T6589C missense mutation in the COI gene (T6589C mtDNA) and the other expressed 40% respiratory activity due to rat (Rattus norvegicus) mtDNAs in mouse cells. By cytoplasmic transfer of these mtDNAs to mouse ES cells, we isolated respiration-deficient ES cells. We obtained chimeric mice and generated their F6 progeny carrying mouse T6589C mtDNAs by its female germ line transmission. They were respiration-deficient and thus could be used as models of mitochondrial diseases caused by point mutations in mtDNA structural genes. However, chimeric mice and mito-mice carrying rat mtDNAs were not obtained, suggesting that significant respiration defects or some deficits induced by rat mtDNAs in mouse ES cells prevented their differentiation to generate mice carrying rat mtDNAs.</abstract><cop>Oxford</cop><pub>Oxford University Press</pub><pmid>16449238</pmid><doi>10.1093/hmg/ddl005</doi><tpages>11</tpages><oa>free_for_read</oa></addata></record>
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subjects	Animals Biological and medical sciences Cell Line Cell Respiration - genetics Chimera Crosses, Genetic DNA, Mitochondrial - genetics Embryonic Stem Cells - metabolism Embryonic Stem Cells - pathology Embryonic Stem Cells - transplantation Female Fundamental and applied biological sciences. Psychology Genetics of eukaryotes. Biological and molecular evolution Male Mice Mice, Inbred BALB C Mice, Inbred C57BL Mice, Inbred ICR Mice, Nude Mice, Transgenic Mitochondria - genetics Molecular and cellular biology Mutation, Missense Phenotype Point Mutation Rats Rats, Wistar Rattus norvegicus
title	Generation of trans-mitochondrial mice carrying homoplasmic mtDNAs with a missense mutation in a structural gene using ES cells
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