Grainyhead 1 Acts As a Drug-inducible Conserved Transcriptional Regulator Linked to Insulin Signaling and Lifespan

Overview

Journal Nat Commun

Specialty Biology

Date 2022 Jan 11

PMID 35013237

Authors

Giovanna Grigolon

Elisa Araldi

Reto Erni

Jia Yee Wu

Carolin Thomas

Marco La Fortezza

Beate Laube

Doris Pohlmann

Markus Stoffel

Kim Zarse

Erick M Carreira

Michael Ristow

Fabian Fischer

Affiliations

Soon will be listed here.

Abstract

Aging is impacted by interventions across species, often converging on metabolic pathways. Transcription factors regulate longevity yet approaches for their pharmacological modulation to exert geroprotection remain sparse. We show that increased expression of the transcription factor Grainyhead 1 (GRH-1) promotes lifespan and pathogen resistance in Caenorhabditis elegans. A compound screen identifies FDA-approved drugs able to activate human GRHL1 and promote nematodal GRH-1-dependent longevity. GRHL1 activity is regulated by post-translational lysine methylation and the phosphoinositide (PI) 3-kinase C2A. Consistently, nematodal longevity following impairment of the PI 3-kinase or insulin/IGF-1 receptor requires grh-1. In BXD mice, Grhl1 expression is positively correlated with lifespan and insulin sensitivity. In humans, GRHL1 expression positively correlates with insulin receptor signaling and also with lifespan. Fasting blood glucose levels, including in individuals with type 2 diabetes, are negatively correlated with GRHL1 expression. Thereby, GRH-1/GRHL1 is identified as a pharmacologically malleable transcription factor impacting insulin signaling and lifespan.

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