4.7 Article

Constraint of gene expression by the chromatin remodelling protein CHD4 facilitates lineage specification

期刊

DEVELOPMENT
卷 142, 期 15, 页码 2586-U90

出版社

COMPANY BIOLOGISTS LTD
DOI: 10.1242/dev.125450

关键词

Lineage commitment; Chromatin remodelling; Blastocyst; Transcription; Trophectoderm; CHD4

资金

  1. BBSRC CASE Studentship in conjunction with Pfizer Neusentis
  2. Wellcome Trust 4-Year PhD Studentship
  3. Wellcome Trust Senior Research Fellowship in the Basic Biomedical Sciences
  4. Wellcome Trust - Medical Research Council Stem Cell Institute

向作者/读者索取更多资源

Chromatin remodelling proteins are essential for different aspects of metazoan biology, yet functional details of why these proteins are important are lacking. Although it is possible to describe the biochemistry of how they remodel chromatin, their chromatin-binding profiles in cell lines, and gene expression changes upon loss of a given protein, in very few cases can this easily translate into an understanding of how the function of that protein actually influences a developmental process. Here, we investigate how the chromatin remodelling protein CHD4 facilitates the first lineage decision in mammalian embryogenesis. Embryos lacking CHD4 can form a morphologically normal early blastocyst, but are unable to successfully complete the first lineage decision and form functional trophectoderm (TE). In the absence of a functional TE, Chd4 mutant blastocysts do not implant and are hence not viable. By measuring transcript levels in single cells from early embryos, we show that CHD4 influences the frequency at which unspecified cells in preimplantation stage embryos express lineage markers prior to the execution of this first lineage decision. In the absence of CHD4, this frequency is increased in 16-cell embryos, and by the blastocyst stage cells fail to properly adopt a TE gene expression programme. We propose that CHD4 allows cells to undertake lineage commitment in vivo by modulating the frequency with which lineage-specification genes are expressed. This provides novel insight into both how lineage decisions are made in mammalian cells, and how a chromatin remodelling protein functions to facilitate lineage commitment.

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