Literature DB >> 36056023

Isoform-specific and ubiquitination dependent recruitment of Tet1 to replicating heterochromatin modulates methylcytosine oxidation.

María Arroyo1, Florian D Hastert2,3, Andreas Zhadan1, Florian Schelter4, Susanne Zimbelmann1, Cathia Rausch1,5, Anne K Ludwig1,6, Thomas Carell4, M Cristina Cardoso7.   

Abstract

Oxidation of the epigenetic DNA mark 5-methylcytosine by Tet dioxygenases is an established route to diversify the epigenetic information, modulate gene expression and overall cellular (patho-)physiology. Here, we demonstrate that Tet1 and its short isoform Tet1s exhibit distinct nuclear localization during DNA replication resulting in aberrant cytosine modification levels in human and mouse cells. We show that Tet1 is tethered away from heterochromatin via its zinc finger domain, which is missing in Tet1s allowing its targeting to these regions. We find that Tet1s interacts with and is ubiquitinated by CRL4(VprBP). The ubiquitinated Tet1s is then recognized by Uhrf1 and recruited to late replicating heterochromatin. This leads to spreading of 5-methylcytosine oxidation to heterochromatin regions, LINE 1 activation and chromatin decondensation. In summary, we elucidate a dual regulation mechanism of Tet1, contributing to the understanding of how epigenetic information can be diversified by spatio-temporal directed Tet1 catalytic activity.
© 2022. The Author(s).

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Year:  2022        PMID: 36056023      PMCID: PMC9440122          DOI: 10.1038/s41467-022-32799-8

Source DB:  PubMed          Journal:  Nat Commun        ISSN: 2041-1723            Impact factor:   17.694


  115 in total

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9.  Developmental differences in genome replication program and origin activation.

Authors:  Cathia Rausch; Patrick Weber; Paulina Prorok; David Hörl; Andreas Maiser; Anne Lehmkuhl; Vadim O Chagin; Corella S Casas-Delucchi; Heinrich Leonhardt; M Cristina Cardoso
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