GADL1 is a multifunctional decarboxylase with tissue-specific roles in β-alanine and carnosine production

Author:

Mahootchi Elaheh,Homaei Selina Cannon,Kleppe Rune,Winge Ingeborg,Hegvik Tor-Arne,Megias-Perez Roberto,Totland Christian,Mogavero Floriana,Baumann Anne,Glennon Jeffrey,Miletic Hrvoje,Kursula Petri,Haavik Jan

Abstract

ABSTRACTCarnosine and related β-alanine-containing peptides are believed to be important antioxidants, pH-buffers and neuromodulators. However, their biosynthetic routes and therapeutic potential are still being debated. This study describes the first animal model lacking the enzyme glutamic acid decarboxylase-like 1 (GADL1). We show that Gadl1-/-mice are deficient in β-alanine, carnosine and anserine, particularly in the olfactory bulb, cerebral cortex, and skeletal muscle. Gadl1-/-mice also exhibited decreased anxiety, increased levels of oxidative stress markers, alterations in energy and lipid metabolism, and age-related changes. Examination of the GADL1 active site indicated that the enzyme may have multiple physiological substrates, including aspartate and cysteine sulfinic acid, compatible with organ-specific functions. Human genetic studies show strong associations of the GADL1 locus with plasma levels of carnosine, subjective well-being, and muscle strength, also indicating a role for β-alanine and its peptide derivatives in these traits. Together, this shows the multifaceted and organ specific roles of carnosine peptides and establishes Gadl1 knockout mice as a versatile model to explore carnosine biology and its therapeutic potential.

Publisher

Cold Spring Harbor Laboratory

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