Hypersensitivity of primordial germ cells to compromised replication-associated DNA repair involves ATM-p53-p21 signaling.

Hypersensitivity of primordial germ cells to compromised replication-associated DNA repair involves ATM-p53-p21 signaling.

Genome maintenance in germ cells is critical for fertility and the stable propagation of species. While mechanisms of meiotic DNA repair and chromosome behavior are well-characterized, the same is not true for primordial germ cells (PGCs), which arise and propagate during very early stages of mammal...

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Main Authors: Yunhai Luo, Suzanne A Hartford, Ruizhu Zeng, Teresa L Southard, Naoko Shima, John C Schimenti
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-07-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC4091704?pdf=render
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spelling doaj-9f08f75606b542ceae80a4632429fbd82020-11-24T22:20:16ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042014-07-01107e100447110.1371/journal.pgen.1004471Hypersensitivity of primordial germ cells to compromised replication-associated DNA repair involves ATM-p53-p21 signaling.Yunhai LuoSuzanne A HartfordRuizhu ZengTeresa L SouthardNaoko ShimaJohn C SchimentiGenome maintenance in germ cells is critical for fertility and the stable propagation of species. While mechanisms of meiotic DNA repair and chromosome behavior are well-characterized, the same is not true for primordial germ cells (PGCs), which arise and propagate during very early stages of mammalian development. Fanconi anemia (FA), a genomic instability syndrome that includes hypogonadism and testicular failure phenotypes, is caused by mutations in genes encoding a complex of proteins involved in repair of DNA lesions associated with DNA replication. The signaling mechanisms underlying hypogonadism and testicular failure in FA patients or mouse models are unknown. We conducted genetic studies to show that hypogonadism of Fancm mutant mice is a result of reduced proliferation, but not apoptosis, of PGCs, resulting in reduced germ cells in neonates of both sexes. Progressive loss of germ cells in adult males also occurs, overlaid with an elevated level of meiotic DNA damage. Genetic studies indicated that ATM-p53-p21 signaling is partially responsible for the germ cell deficiency.http://europepmc.org/articles/PMC4091704?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Yunhai Luo
Suzanne A Hartford
Ruizhu Zeng
Teresa L Southard
Naoko Shima
John C Schimenti
spellingShingle Yunhai Luo
Suzanne A Hartford
Ruizhu Zeng
Teresa L Southard
Naoko Shima
John C Schimenti
Hypersensitivity of primordial germ cells to compromised replication-associated DNA repair involves ATM-p53-p21 signaling.
PLoS Genetics
author_facet Yunhai Luo
Suzanne A Hartford
Ruizhu Zeng
Teresa L Southard
Naoko Shima
John C Schimenti
author_sort Yunhai Luo
title Hypersensitivity of primordial germ cells to compromised replication-associated DNA repair involves ATM-p53-p21 signaling.
title_short Hypersensitivity of primordial germ cells to compromised replication-associated DNA repair involves ATM-p53-p21 signaling.
title_full Hypersensitivity of primordial germ cells to compromised replication-associated DNA repair involves ATM-p53-p21 signaling.
title_fullStr Hypersensitivity of primordial germ cells to compromised replication-associated DNA repair involves ATM-p53-p21 signaling.
title_full_unstemmed Hypersensitivity of primordial germ cells to compromised replication-associated DNA repair involves ATM-p53-p21 signaling.
title_sort hypersensitivity of primordial germ cells to compromised replication-associated dna repair involves atm-p53-p21 signaling.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2014-07-01
description Genome maintenance in germ cells is critical for fertility and the stable propagation of species. While mechanisms of meiotic DNA repair and chromosome behavior are well-characterized, the same is not true for primordial germ cells (PGCs), which arise and propagate during very early stages of mammalian development. Fanconi anemia (FA), a genomic instability syndrome that includes hypogonadism and testicular failure phenotypes, is caused by mutations in genes encoding a complex of proteins involved in repair of DNA lesions associated with DNA replication. The signaling mechanisms underlying hypogonadism and testicular failure in FA patients or mouse models are unknown. We conducted genetic studies to show that hypogonadism of Fancm mutant mice is a result of reduced proliferation, but not apoptosis, of PGCs, resulting in reduced germ cells in neonates of both sexes. Progressive loss of germ cells in adult males also occurs, overlaid with an elevated level of meiotic DNA damage. Genetic studies indicated that ATM-p53-p21 signaling is partially responsible for the germ cell deficiency.
url http://europepmc.org/articles/PMC4091704?pdf=render
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AT suzanneahartford hypersensitivityofprimordialgermcellstocompromisedreplicationassociateddnarepairinvolvesatmp53p21signaling
AT ruizhuzeng hypersensitivityofprimordialgermcellstocompromisedreplicationassociateddnarepairinvolvesatmp53p21signaling
AT teresalsouthard hypersensitivityofprimordialgermcellstocompromisedreplicationassociateddnarepairinvolvesatmp53p21signaling
AT naokoshima hypersensitivityofprimordialgermcellstocompromisedreplicationassociateddnarepairinvolvesatmp53p21signaling
AT johncschimenti hypersensitivityofprimordialgermcellstocompromisedreplicationassociateddnarepairinvolvesatmp53p21signaling
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