Mouse zygotes respond to severe sperm DNA damage by delaying paternal DNA replication and embryonic development.

Mouse zygotes respond to severe sperm DNA damage by delaying paternal DNA replication and embryonic development.

Mouse zygotes do not activate apoptosis in response to DNA damage. We previously reported a unique form of inducible sperm DNA damage termed sperm chromatin fragmentation (SCF). SCF mirrors some aspects of somatic cell apoptosis in that the DNA degradation is mediated by reversible double strand bre...

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Main Authors: Joanna E Gawecka, Joel Marh, Michael Ortega, Yasuhiro Yamauchi, Monika A Ward, W Steven Ward
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3576397?pdf=render
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spelling doaj-1b5927ff67da447895c7cd543ab3d63d2020-11-25T02:47:26ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0182e5638510.1371/journal.pone.0056385Mouse zygotes respond to severe sperm DNA damage by delaying paternal DNA replication and embryonic development.Joanna E GaweckaJoel MarhMichael OrtegaYasuhiro YamauchiMonika A WardW Steven WardMouse zygotes do not activate apoptosis in response to DNA damage. We previously reported a unique form of inducible sperm DNA damage termed sperm chromatin fragmentation (SCF). SCF mirrors some aspects of somatic cell apoptosis in that the DNA degradation is mediated by reversible double strand breaks caused by topoisomerase 2B (TOP2B) followed by irreversible DNA degradation by a nuclease(s). Here, we created zygotes using spermatozoa induced to undergo SCF (SCF zygotes) and tested how they responded to moderate and severe paternal DNA damage during the first cell cycle. We found that the TUNEL assay was not sensitive enough to identify the breaks caused by SCF in zygotes in either case. However, paternal pronuclei in both groups stained positively for γH2AX, a marker for DNA damage, at 5 hrs after fertilization, just before DNA synthesis, while the maternal pronuclei were negative. We also found that both pronuclei in SCF zygotes with moderate DNA damage replicated normally, but paternal pronuclei in the SCF zygotes with severe DNA damage delayed the initiation of DNA replication by up to 12 hrs even though the maternal pronuclei had no discernable delay. Chromosomal analysis of both groups confirmed that the paternal DNA was degraded after S-phase while the maternal pronuclei formed normal chromosomes. The DNA replication delay caused a marked retardation in progression to the 2-cell stage, and a large portion of the embryos arrested at the G2/M border, suggesting that this is an important checkpoint in zygotic development. Those embryos that progressed through the G2/M border died at later stages and none developed to the blastocyst stage. Our data demonstrate that the zygote responds to sperm DNA damage through a non-apoptotic mechanism that acts by slowing paternal DNA replication and ultimately leads to arrest in embryonic development.http://europepmc.org/articles/PMC3576397?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Joanna E Gawecka
Joel Marh
Michael Ortega
Yasuhiro Yamauchi
Monika A Ward
W Steven Ward
spellingShingle Joanna E Gawecka
Joel Marh
Michael Ortega
Yasuhiro Yamauchi
Monika A Ward
W Steven Ward
Mouse zygotes respond to severe sperm DNA damage by delaying paternal DNA replication and embryonic development.
PLoS ONE
author_facet Joanna E Gawecka
Joel Marh
Michael Ortega
Yasuhiro Yamauchi
Monika A Ward
W Steven Ward
author_sort Joanna E Gawecka
title Mouse zygotes respond to severe sperm DNA damage by delaying paternal DNA replication and embryonic development.
title_short Mouse zygotes respond to severe sperm DNA damage by delaying paternal DNA replication and embryonic development.
title_full Mouse zygotes respond to severe sperm DNA damage by delaying paternal DNA replication and embryonic development.
title_fullStr Mouse zygotes respond to severe sperm DNA damage by delaying paternal DNA replication and embryonic development.
title_full_unstemmed Mouse zygotes respond to severe sperm DNA damage by delaying paternal DNA replication and embryonic development.
title_sort mouse zygotes respond to severe sperm dna damage by delaying paternal dna replication and embryonic development.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Mouse zygotes do not activate apoptosis in response to DNA damage. We previously reported a unique form of inducible sperm DNA damage termed sperm chromatin fragmentation (SCF). SCF mirrors some aspects of somatic cell apoptosis in that the DNA degradation is mediated by reversible double strand breaks caused by topoisomerase 2B (TOP2B) followed by irreversible DNA degradation by a nuclease(s). Here, we created zygotes using spermatozoa induced to undergo SCF (SCF zygotes) and tested how they responded to moderate and severe paternal DNA damage during the first cell cycle. We found that the TUNEL assay was not sensitive enough to identify the breaks caused by SCF in zygotes in either case. However, paternal pronuclei in both groups stained positively for γH2AX, a marker for DNA damage, at 5 hrs after fertilization, just before DNA synthesis, while the maternal pronuclei were negative. We also found that both pronuclei in SCF zygotes with moderate DNA damage replicated normally, but paternal pronuclei in the SCF zygotes with severe DNA damage delayed the initiation of DNA replication by up to 12 hrs even though the maternal pronuclei had no discernable delay. Chromosomal analysis of both groups confirmed that the paternal DNA was degraded after S-phase while the maternal pronuclei formed normal chromosomes. The DNA replication delay caused a marked retardation in progression to the 2-cell stage, and a large portion of the embryos arrested at the G2/M border, suggesting that this is an important checkpoint in zygotic development. Those embryos that progressed through the G2/M border died at later stages and none developed to the blastocyst stage. Our data demonstrate that the zygote responds to sperm DNA damage through a non-apoptotic mechanism that acts by slowing paternal DNA replication and ultimately leads to arrest in embryonic development.
url http://europepmc.org/articles/PMC3576397?pdf=render
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AT michaelortega mousezygotesrespondtoseverespermdnadamagebydelayingpaternaldnareplicationandembryonicdevelopment
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