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Obtaining mice that carry human mitochondrial DNA transmitted to the progeny

To study human diseases associated with mutations in mitochondrial DNA one needs an animal model in which the distribution of abnormal mtDNA and its impact on the phenotype might be followed. We isolated human mitochondria from HepG2 cell culture and microinjected them into murine zygotes, upon whic...

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Published in:	Molecular reproduction and development 2004-07, Vol.68 (3), p.299-307
Main Authors:	Sokolova, Vassilina A., Kustova, Maria E., Arbuzova, Natalia I., Sorokin, Alexander V., Moskaliova, Olesya S., Bass, Mikhail G., Vasilyev, Vadim B.
Format:	Article
Language:	English
Subjects:	Animals Cell Line, Tumor DNA, Mitochondrial - genetics Embryo, Mammalian - metabolism Extrachromosomal Inheritance Female Gene Transfer Techniques human mtDNA Humans Male maternal inheritance Mice Mice, Inbred C57BL Mice, Transgenic Microinjections Mitochondria - genetics mitochondria microinjection mtDNA transfer Mutation Organ Specificity Polymerase Chain Reaction Pregnancy Pseudopregnancy transgenic mice Zygote - transplantation Zygote - ultrastructure
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cited_by	cdi_FETCH-LOGICAL-c3905-1eb54780ea1726fc2a93e00882631540bc925f1cf4ab573d46cb887f2f6fb82d3
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container_title	Molecular reproduction and development
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creator	Sokolova, Vassilina A. Kustova, Maria E. Arbuzova, Natalia I. Sorokin, Alexander V. Moskaliova, Olesya S. Bass, Mikhail G. Vasilyev, Vadim B.
description	To study human diseases associated with mutations in mitochondrial DNA one needs an animal model in which the distribution of abnormal mtDNA and its impact on the phenotype might be followed. We isolated human mitochondria from HepG2 cell culture and microinjected them into murine zygotes, upon which those were transplanted to the pseudopregnant mice. PCR with species‐specific primers allowed detecting human mtDNA in the tissues of 7–13‐day embryos. No serious alterations in the development of transmitochondrial embryos were noticed. Among various organs/tissues of the 13‐day embryos, human mtDNA was detected only in the heart, skeletal muscles, and stomach, which is in line with its uneven distribution among the blastomeres of an early mouse embryo that we described previously. In four recipient females, the microinjected zygotes were allowed to develop to term, the four neonate males of their joint litter were sacrificed, and in three of them human mtDNA was detected in the heart, skeletal muscles, stomach, brain, testes, and bladder. Six females of that joint litter were grown and mated to intact males. In the progeny (F1) of one of the females two mice were carrying human mtDNA in the heart, skeletal muscles, stomach, brain, lungs, uterus, ovaries, and kidneys. The study confirms the possibility to obtain transmitochondrial mice carrying human mtDNA that is transmitted to the animals of the next generation. Our results also indicate that among the organs to which human mtDNA is distributed some are more likely to receive it than others. Mol. Reprod. Dev. 68: 299–307, 2004. © 2004 Wiley‐Liss, Inc.
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We isolated human mitochondria from HepG2 cell culture and microinjected them into murine zygotes, upon which those were transplanted to the pseudopregnant mice. PCR with species‐specific primers allowed detecting human mtDNA in the tissues of 7–13‐day embryos. No serious alterations in the development of transmitochondrial embryos were noticed. Among various organs/tissues of the 13‐day embryos, human mtDNA was detected only in the heart, skeletal muscles, and stomach, which is in line with its uneven distribution among the blastomeres of an early mouse embryo that we described previously. In four recipient females, the microinjected zygotes were allowed to develop to term, the four neonate males of their joint litter were sacrificed, and in three of them human mtDNA was detected in the heart, skeletal muscles, stomach, brain, testes, and bladder. Six females of that joint litter were grown and mated to intact males. 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Reprod. Dev</addtitle><description>To study human diseases associated with mutations in mitochondrial DNA one needs an animal model in which the distribution of abnormal mtDNA and its impact on the phenotype might be followed. We isolated human mitochondria from HepG2 cell culture and microinjected them into murine zygotes, upon which those were transplanted to the pseudopregnant mice. PCR with species‐specific primers allowed detecting human mtDNA in the tissues of 7–13‐day embryos. No serious alterations in the development of transmitochondrial embryos were noticed. Among various organs/tissues of the 13‐day embryos, human mtDNA was detected only in the heart, skeletal muscles, and stomach, which is in line with its uneven distribution among the blastomeres of an early mouse embryo that we described previously. 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Dev. 68: 299–307, 2004. © 2004 Wiley‐Liss, Inc.</description><subject>Animals</subject><subject>Cell Line, Tumor</subject><subject>DNA, Mitochondrial - genetics</subject><subject>Embryo, Mammalian - metabolism</subject><subject>Extrachromosomal Inheritance</subject><subject>Female</subject><subject>Gene Transfer Techniques</subject><subject>human mtDNA</subject><subject>Humans</subject><subject>Male</subject><subject>maternal inheritance</subject><subject>Mice</subject><subject>Mice, Inbred C57BL</subject><subject>Mice, Transgenic</subject><subject>Microinjections</subject><subject>Mitochondria - genetics</subject><subject>mitochondria microinjection</subject><subject>mtDNA transfer</subject><subject>Mutation</subject><subject>Organ Specificity</subject><subject>Polymerase Chain Reaction</subject><subject>Pregnancy</subject><subject>Pseudopregnancy</subject><subject>transgenic mice</subject><subject>Zygote - transplantation</subject><subject>Zygote - ultrastructure</subject><issn>1040-452X</issn><issn>1098-2795</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2004</creationdate><recordtype>article</recordtype><recordid>eNqFkMtOwzAQRS0E4r3gB1BWSCwCYzuOnWVpeaoUCYHoznIcpw3kUWxX0L_H0AIrxGpGo3PvSAehAwwnGICcNrY4IQCcraFtDJmICc_Y-ueeQJwwMt5CO849A0CWCdhEW5hhTCgh22h4l3tVtVU7iZpKm8hPlY-0snYRTeeNasPVd3ratYWtVB0NRr3IW9W6cPamiHwXEiaa2W5i2sUe2ihV7cz-au6ix4vzh_5VPLy7vO73hrGmGbAYm5wlXIBRmJO01ERl1AAIQVKKWQK5zggrsS4TlTNOiyTVuRC8JGVa5oIUdBcdLXvD39e5cV42ldOmrlVrurmTHAvOOBP_glgASQgnATxegtp2zllTypmtGmUXEoP8dCyDY_nlOLCHq9J53pjil1xJDcDpEnirarP4u0ne3g--K-NlonLevP8klH2RKaeBfBpdSjoe05tRciYf6AdaXpQ3</recordid><startdate>200407</startdate><enddate>200407</enddate><creator>Sokolova, Vassilina A.</creator><creator>Kustova, Maria E.</creator><creator>Arbuzova, Natalia I.</creator><creator>Sorokin, Alexander V.</creator><creator>Moskaliova, Olesya S.</creator><creator>Bass, Mikhail G.</creator><creator>Vasilyev, Vadim B.</creator><general>Wiley Subscription Services, Inc., A Wiley Company</general><scope>BSCLL</scope><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>8FD</scope><scope>FR3</scope><scope>P64</scope><scope>RC3</scope><scope>7X8</scope></search><sort><creationdate>200407</creationdate><title>Obtaining mice that carry human mitochondrial DNA transmitted to the progeny</title><author>Sokolova, Vassilina A. ; 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subjects	Animals Cell Line, Tumor DNA, Mitochondrial - genetics Embryo, Mammalian - metabolism Extrachromosomal Inheritance Female Gene Transfer Techniques human mtDNA Humans Male maternal inheritance Mice Mice, Inbred C57BL Mice, Transgenic Microinjections Mitochondria - genetics mitochondria microinjection mtDNA transfer Mutation Organ Specificity Polymerase Chain Reaction Pregnancy Pseudopregnancy transgenic mice Zygote - transplantation Zygote - ultrastructure
title	Obtaining mice that carry human mitochondrial DNA transmitted to the progeny
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