Literature DB >> 32359405

Myt Transcription Factors Prevent Stress-Response Gene Overactivation to Enable Postnatal Pancreatic β Cell Proliferation, Function, and Survival.

Ruiying Hu1, Emily Walker2, Chen Huang1, Yanwen Xu1, Chen Weng3, Gillian E Erickson1, Anastasia Coldren4, Xiaodun Yang1, Marcela Brissova4, Irina Kaverina1, Appakalai N Balamurugan5, Christopher V E Wright1, Yan Li3, Roland Stein2, Guoqiang Gu6.   

Abstract

Although cellular stress response is important for maintaining function and survival, overactivation of late-stage stress effectors cause dysfunction and death. We show that the myelin transcription factors (TFs) Myt1 (Nzf2), Myt2 (Myt1l, Nztf1, and Png-1), and Myt3 (St18 and Nzf3) prevent such overactivation in islet β cells. Thus, we found that co-inactivating the Myt TFs in mouse pancreatic progenitors compromised postnatal β cell function, proliferation, and survival, preceded by upregulation of late-stage stress-response genes activating transcription factors (e.g., Atf4) and heat-shock proteins (Hsps). Myt1 binds putative enhancers of Atf4 and Hsps, whose overexpression largely recapitulated the Myt-mutant phenotypes. Moreover, Myt(MYT)-TF levels were upregulated in mouse and human β cells during metabolic stress-induced compensation but downregulated in dysfunctional type 2 diabetic (T2D) human β cells. Lastly, MYT knockdown caused stress-gene overactivation and death in human EndoC-βH1 cells. These findings suggest that Myt TFs are essential restrictors of stress-response overactivity.
Copyright © 2020 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  ATF4; Myelin transcription factors; beta cell compensation; beta cell death; beta cell failure; diabetes; heat-shock proteins; post-transcriptional control; proliferation; stress response

Mesh:

Substances:

Year:  2020        PMID: 32359405      PMCID: PMC7278035          DOI: 10.1016/j.devcel.2020.04.003

Source DB:  PubMed          Journal:  Dev Cell        ISSN: 1534-5807            Impact factor:   12.270


  67 in total

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2.  Microtubules and Gαo-signaling modulate the preferential secretion of young insulin secretory granules in islet β cells via independent pathways.

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Journal:  PLoS One       Date:  2021-07-22       Impact factor: 3.240

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