Literature DB >> 15581869

Distinct dynamics and distribution of histone methyl-lysine derivatives in mouse development.

Vincent L Biron1, Kirk J McManus, Ninghe Hu, Michael J Hendzel, D Alan Underhill.   

Abstract

Histone methylation acts as an epigenetic regulator of chromatin activity through the modification of arginine and lysine residues on histones H3 and H4. In the case of lysine, this includes the formation of mono-, di-, or trimethyl groups, each of which is presumed to represent a distinct functional state at the cellular level. To examine the potential developmental roles of these modifications, we determined the global patterns of lysine methylation involving K9 on histone H3 and K20 on histone H4 in midgestation mouse embryos. For each lysine target site, we observed distinct subnuclear distributions of the mono- and trimethyl versions in 10T1/2 cells that were conserved within primary cultures and within the 3D-tissue architecture of the embryo. Interestingly, three of these modifications, histone H3 trimethyl K9, histone H4 monomethyl K20, and histone H4 trimethyl K20 exhibited marked differences in their distribution within the neuroepithelium. Specifically, both histone H3 trimethyl K9 and H4 monomethyl K20 were elevated in proliferating cells of the neural tube, which in the case of the K9 modification was limited to mitotic cells on the luminal surface. In contrast, histone H4 trimethyl K20 was progressively lost from these medial regions and became enriched in differentiating neurons in the ventrolateral neural tube. The inverse relationship of histone H4 K20 methyl derivatives is even more striking during skeletal and cardiac myogenesis where the accumulation of the trimethyl modification in pericentromeric heterochromatin suggests a role in gene silencing in postmitotic muscle cells. Importantly, our results establish that histone lysine methylation occurs in a highly dynamic manner that is consistent with their function in an epigenetic program for cell division and differentiation.

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Year:  2004        PMID: 15581869     DOI: 10.1016/j.ydbio.2004.08.038

Source DB:  PubMed          Journal:  Dev Biol        ISSN: 0012-1606            Impact factor:   3.582


  22 in total

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Review 2.  Towards incorporating epigenetic mechanisms into carcinogen identification and evaluation.

Authors:  Zdenko Herceg; Marie-Pierre Lambert; Karin van Veldhoven; Christiana Demetriou; Paolo Vineis; Martyn T Smith; Kurt Straif; Christopher P Wild
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3.  In situ histone landscape of nephrogenesis.

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Journal:  Epigenetics       Date:  2013-10-29       Impact factor: 4.528

4.  PR-Set7 establishes a repressive trans-tail histone code that regulates differentiation.

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Review 5.  Epigenetic modifications in 3D: nuclear organization of the differentiating mammary epithelial cell.

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Review 6.  Epigenetic States of nephron progenitors and epithelial differentiation.

Authors:  Mazhar Adli; Mahmut Parlak; Yuwen Li; Samir S El-Dahr
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7.  Dynamic shifts in chromatin states differentially mark the proliferative basal cells and terminally differentiated cells of the developing epidermis.

Authors:  Yan Ting Shue; Kang Ting Lee; Benjamin William Walters; Hui Binn Ong; Shaktheeshwari Silvaraju; Wei Jun Lam; Chin Yan Lim
Journal:  Epigenetics       Date:  2020-03-16       Impact factor: 4.528

Review 8.  An epigenetic perspective on the free radical theory of development.

Authors:  Michael J Hitchler; Frederick E Domann
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Review 9.  Epigenetic regulation in human brain-focus on histone lysine methylation.

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Journal:  Biol Psychiatry       Date:  2008-09-24       Impact factor: 13.382

Review 10.  Epigenetics mechanisms in renal development.

Authors:  Sylvia A Hilliard; Samir S El-Dahr
Journal:  Pediatr Nephrol       Date:  2015-10-22       Impact factor: 3.714

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