TFEB and TFE3 control glucose homeostasis by regulating insulin gene expression-Reference-Cited by-同舟云学术

TFEB and TFE3 control glucose homeostasis by regulating insulin gene expression

Published:2023-09-15 Issue:21 Volume:42 Page:
ISSN:0261-4189
Container-title:The EMBO Journal
language:en
Short-container-title:The EMBO Journal

Author:

Pasquier Adrien¹^ORCID,Pastore Nunzia¹²^ORCID,D'Orsi Luca¹,Colonna Rita¹,Esposito Alessandra¹^ORCID,Maffia Veronica¹,De Cegli Rossella¹^ORCID,Mutarelli Margherita³^ORCID,Ambrosio Susanna¹,Tufano Gennaro¹^ORCID,Grimaldi Antonio¹,Cesana Marcella¹,Cacchiarelli Davide¹²⁴,Delalleau Nathalie⁵⁶,Napolitano Gennaro¹²⁴^ORCID,Ballabio Andrea¹²⁴⁷⁸^ORCID

Affiliation:

1. Telethon Institute of Genetics and Medicine (TIGEM) Naples Italy

2. Medical Genetics Unit, Department of Medical and Translational Science Federico II University Naples Italy

3. Institute of Applied Sciences and Intelligent Systems National Research Council (ISASI‐CNR) Pozzuoli Italy

4. School for Advanced Studies, Genomics and Experimental Medicine Program University of Naples "Federico II" Naples Italy

5. University of Lille, U1190‐EGID Lille France

6. Inserm, U1190 Lille France

7. Department of Molecular and Human Genetics Baylor College of Medicine Houston TX USA

8. Jan and Dan Duncan Neurological Research Institute Texas Children's Hospital Houston TX USA

Abstract

AbstractTo fulfill their function, pancreatic beta cells require precise nutrient‐sensing mechanisms that control insulin production. Transcription factor EB (TFEB) and its homolog TFE3 have emerged as crucial regulators of the adaptive response of cell metabolism to environmental cues. Here, we show that TFEB and TFE3 regulate beta‐cell function and insulin gene expression in response to variations in nutrient availability. We found that nutrient deprivation in beta cells promoted TFEB/TFE3 activation, which resulted in suppression of insulin gene expression. TFEB overexpression was sufficient to inhibit insulin transcription, whereas beta cells depleted of both TFEB and TFE3 failed to suppress insulin gene expression in response to amino acid deprivation. Interestingly, ChIP‐seq analysis showed binding of TFEB to super‐enhancer regions that regulate insulin transcription. Conditional, beta‐cell‐specific, Tfeb‐overexpressing, and Tfeb/Tfe3 double‐KO mice showed severe alteration of insulin transcription, secretion, and glucose tolerance, indicating that TFEB and TFE3 are important physiological mediators of pancreatic function. Our findings reveal a nutrient‐controlled transcriptional mechanism that regulates insulin production, thus playing a key role in glucose homeostasis at both cellular and organismal levels.

Funder

European Foundation for the Study of Diabetes

Fondation pour la Recherche Médicale

Fondazione Telethon

Publisher

Springer Science and Business Media LLC

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,Molecular Biology,General Neuroscience

Link

https://www.embopress.org/doi/pdf/10.15252/embj.2023113928

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