Vitamin B2 Enables Regulation of Fasting Glucose Availability

Overview

Journal Elife

Specialty Biology

Date 2023 Jul 7

PMID 37417957

Authors

Peter M Masschelin

Pradip Saha

Scott A Ochsner

Aaron R Cox

Kang Ho Kim

Jessica B Felix

Robert Sharp

Xin Li

Lin Tan

Jun Hyoung Park

Liping Wang

Vasanta Putluri

Philip L Lorenzi

Alli M Nuotio-Antar

Zheng Sun

Benny Abraham Kaipparettu

Nagireddy Putluri

David D Moore

Scott A Summers

Neil J McKenna

Sean M Hartig

Affiliations

Soon will be listed here.

Abstract

Flavin adenine dinucleotide (FAD) interacts with flavoproteins to mediate oxidation-reduction reactions required for cellular energy demands. Not surprisingly, mutations that alter FAD binding to flavoproteins cause rare inborn errors of metabolism (IEMs) that disrupt liver function and render fasting intolerance, hepatic steatosis, and lipodystrophy. In our study, depleting FAD pools in mice with a vitamin B2-deficient diet (B2D) caused phenotypes associated with organic acidemias and other IEMs, including reduced body weight, hypoglycemia, and fatty liver disease. Integrated discovery approaches revealed B2D tempered fasting activation of target genes for the nuclear receptor PPARα, including those required for gluconeogenesis. We also found PPARα knockdown in the liver recapitulated B2D effects on glucose excursion and fatty liver disease in mice. Finally, treatment with the PPARα agonist fenofibrate activated the integrated stress response and refilled amino acid substrates to rescue fasting glucose availability and overcome B2D phenotypes. These findings identify metabolic responses to FAD availability and nominate strategies for the management of organic acidemias and other rare IEMs.

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