Variation in germ line mtDNA heteroplasmy is determined prenatally but modified during subsequent transmission

A genetic bottleneck explains the marked changes in mitochondrial DNA (mtDNA) heteroplasmy observed during the transmission of pathogenic mutations, but the precise timing remains controversial, and it is not clear whether selection plays a role. These issues are critically important for the genetic...

Descripción completa

Detalles Bibliográficos
Autores principales: Freyer, Christoph, Cree, Lynsey M., Mourier, Arnaud, Stewart, James B., Koolmeister, Camilla, Milenkovic, Dusanka, Wai, Timothy, Floros, Vasileios I., Hagström, Erik, Chatzidaki, Emmanouella E., Wiesner, Rudolph J., Samuels, David C, Larsson, Nils-Göran, Chinnery, Patrick F.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2012
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3492742/
https://www.ncbi.nlm.nih.gov/pubmed/23042113
http://dx.doi.org/10.1038/ng.2427
_version_ 1782249162283155456
author Freyer, Christoph
Cree, Lynsey M.
Mourier, Arnaud
Stewart, James B.
Koolmeister, Camilla
Milenkovic, Dusanka
Wai, Timothy
Floros, Vasileios I.
Hagström, Erik
Chatzidaki, Emmanouella E.
Wiesner, Rudolph J.
Samuels, David C
Larsson, Nils-Göran
Chinnery, Patrick F.
author_facet Freyer, Christoph
Cree, Lynsey M.
Mourier, Arnaud
Stewart, James B.
Koolmeister, Camilla
Milenkovic, Dusanka
Wai, Timothy
Floros, Vasileios I.
Hagström, Erik
Chatzidaki, Emmanouella E.
Wiesner, Rudolph J.
Samuels, David C
Larsson, Nils-Göran
Chinnery, Patrick F.
author_sort Freyer, Christoph
collection PubMed
description A genetic bottleneck explains the marked changes in mitochondrial DNA (mtDNA) heteroplasmy observed during the transmission of pathogenic mutations, but the precise timing remains controversial, and it is not clear whether selection plays a role. These issues are critically important for the genetic counseling of prospective mothers, and developing treatments aimed at disease prevention. By studying mice transmitting a heteroplasmic single base-pair deletion in the mitochondrial tRNA(Met) gene, we show that mammalian mtDNA heteroplasmy levels are principally determined prenatally within the developing female germ line. Although we saw no evidence of mtDNA selection prenatally, skewed heteroplasmy levels were observed in the offspring of the next generation, consistent with purifying selection. High percentage levels of the tRNA(Met) mutation were linked to a compensatory increase in overall mitochondrial RNAs, ameliorating the biochemical phenotype, and explaining why fecundity is not compromised.
format Online
Article
Text
id pubmed-3492742
institution National Center for Biotechnology Information
language English
publishDate 2012
record_format MEDLINE/PubMed
spelling pubmed-34927422013-05-01 Variation in germ line mtDNA heteroplasmy is determined prenatally but modified during subsequent transmission Freyer, Christoph Cree, Lynsey M. Mourier, Arnaud Stewart, James B. Koolmeister, Camilla Milenkovic, Dusanka Wai, Timothy Floros, Vasileios I. Hagström, Erik Chatzidaki, Emmanouella E. Wiesner, Rudolph J. Samuels, David C Larsson, Nils-Göran Chinnery, Patrick F. Nat Genet Article A genetic bottleneck explains the marked changes in mitochondrial DNA (mtDNA) heteroplasmy observed during the transmission of pathogenic mutations, but the precise timing remains controversial, and it is not clear whether selection plays a role. These issues are critically important for the genetic counseling of prospective mothers, and developing treatments aimed at disease prevention. By studying mice transmitting a heteroplasmic single base-pair deletion in the mitochondrial tRNA(Met) gene, we show that mammalian mtDNA heteroplasmy levels are principally determined prenatally within the developing female germ line. Although we saw no evidence of mtDNA selection prenatally, skewed heteroplasmy levels were observed in the offspring of the next generation, consistent with purifying selection. High percentage levels of the tRNA(Met) mutation were linked to a compensatory increase in overall mitochondrial RNAs, ameliorating the biochemical phenotype, and explaining why fecundity is not compromised. 2012-10-07 2012-11 /pmc/articles/PMC3492742/ /pubmed/23042113 http://dx.doi.org/10.1038/ng.2427 Text en Users may view, print, copy, download and text and data- mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Freyer, Christoph
Cree, Lynsey M.
Mourier, Arnaud
Stewart, James B.
Koolmeister, Camilla
Milenkovic, Dusanka
Wai, Timothy
Floros, Vasileios I.
Hagström, Erik
Chatzidaki, Emmanouella E.
Wiesner, Rudolph J.
Samuels, David C
Larsson, Nils-Göran
Chinnery, Patrick F.
Variation in germ line mtDNA heteroplasmy is determined prenatally but modified during subsequent transmission
title Variation in germ line mtDNA heteroplasmy is determined prenatally but modified during subsequent transmission
title_full Variation in germ line mtDNA heteroplasmy is determined prenatally but modified during subsequent transmission
title_fullStr Variation in germ line mtDNA heteroplasmy is determined prenatally but modified during subsequent transmission
title_full_unstemmed Variation in germ line mtDNA heteroplasmy is determined prenatally but modified during subsequent transmission
title_short Variation in germ line mtDNA heteroplasmy is determined prenatally but modified during subsequent transmission
title_sort variation in germ line mtdna heteroplasmy is determined prenatally but modified during subsequent transmission
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3492742/
https://www.ncbi.nlm.nih.gov/pubmed/23042113
http://dx.doi.org/10.1038/ng.2427
work_keys_str_mv AT freyerchristoph variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT creelynseym variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT mourierarnaud variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT stewartjamesb variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT koolmeistercamilla variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT milenkovicdusanka variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT waitimothy variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT florosvasileiosi variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT hagstromerik variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT chatzidakiemmanouellae variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT wiesnerrudolphj variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT samuelsdavidc variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT larssonnilsgoran variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission
AT chinnerypatrickf variationingermlinemtdnaheteroplasmyisdeterminedprenatallybutmodifiedduringsubsequenttransmission

Ejemplares similares