Literature DB >> 29358330

Histone variant H3.3-mediated chromatin remodeling is essential for paternal genome activation in mouse preimplantation embryos.

Qingran Kong1,2, Laura A Banaszynski3, Fuqiang Geng4, Xiaolei Zhang2, Jiaming Zhang2, Heng Zhang2, Claire L O'Neill1, Peidong Yan2, Zhonghua Liu2, Koji Shido4, Gianpiero D Palermo1, C David Allis3, Shahin Rafii4, Zev Rosenwaks1, Duancheng Wen5.   

Abstract

Derepression of chromatin-mediated transcriptional repression of paternal and maternal genomes is considered the first major step that initiates zygotic gene expression after fertilization. The histone variant H3.3 is present in both male and female gametes and is thought to be important for remodeling the paternal and maternal genomes for activation during both fertilization and embryogenesis. However, the underlying mechanisms remain poorly understood. Using our H3.3B-HA-tagged mouse model, engineered to report H3.3 expression in live animals and to distinguish different sources of H3.3 protein in embryos, we show here that sperm-derived H3.3 (sH3.3) protein is removed from the sperm genome shortly after fertilization and extruded from the zygotes via the second polar bodies (PBII) during embryogenesis. We also found that the maternal H3.3 (mH3.3) protein is incorporated into the paternal genome as early as 2 h postfertilization and is detectable in the paternal genome until the morula stage. Knockdown of maternal H3.3 resulted in compromised embryonic development both of fertilized embryos and of androgenetic haploid embryos. Furthermore, we report that mH3.3 depletion in oocytes impairs both activation of the Oct4 pluripotency marker gene and global de novo transcription from the paternal genome important for early embryonic development. Our results suggest that H3.3-mediated paternal chromatin remodeling is essential for the development of preimplantation embryos and the activation of the paternal genome during embryogenesis.
© 2018 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  chromatin remodeling; development; embryo; embryogenesis; embryonic development; epigenetic reprogramming; epigenetics; fertilization; gene expression; histone; histone variant H3.3; oocyte; paternal genome activation; sperm; transcriptional repression

Mesh:

Substances:

Year:  2018        PMID: 29358330      PMCID: PMC5846143          DOI: 10.1074/jbc.RA117.001150

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  52 in total

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Authors:  Ray Kit Ng; J B Gurdon
Journal:  Nat Cell Biol       Date:  2007-12-09       Impact factor: 28.824

2.  Genome editing a mouse locus encoding a variant histone, H3.3B, to report on its expression in live animals.

Authors:  Duancheng Wen; Kyung-Min Noh; Aaron D Goldberg; C David Allis; Zev Rosenwaks; Shahin Rafii; Laura A Banaszynski
Journal:  Genesis       Date:  2014-10-06       Impact factor: 2.487

3.  Nucleosome assembly is required for nuclear pore complex assembly in mouse zygotes.

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Journal:  Nature       Date:  2012-09-30       Impact factor: 49.962

5.  Rapid replacement of somatic linker histones with the oocyte-specific linker histone H1foo in nuclear transfer.

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Review 6.  Restarting life: fertilization and the transition from meiosis to mitosis.

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Authors:  Miler T Lee; Ashley R Bonneau; Carter M Takacs; Ariel A Bazzini; Kate R DiVito; Elizabeth S Fleming; Antonio J Giraldez
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10.  Inferring the choreography of parental genomes during fertilization from ultralarge-scale whole-transcriptome analysis.

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3.  H3.3 Nucleosome Assembly Mutants Display a Late-Onset Maternal Effect.

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Review 5.  Listening to mother: Long-term maternal effects in mammalian development.

Authors:  Meghan L Ruebel; Keith E Latham
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Review 7.  Heterochromatin Morphodynamics in Late Oogenesis and Early Embryogenesis of Mammals.

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9.  Histone H3.3 phosphorylation amplifies stimulation-induced transcription.

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Journal:  Nature       Date:  2020-07-22       Impact factor: 49.962

10.  Differential Expression of Histone H3.3 Genes and Their Role in Modulating Temperature Stress Response in Caenorhabditis elegans.

Authors:  Kamila Delaney; Jonathan Mailler; Joanna M Wenda; Caroline Gabus; Florian A Steiner
Journal:  Genetics       Date:  2018-04-10       Impact factor: 4.562

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