A PTER-dependent pathway of taurine metabolism linked to energy balance

Author:

Wei WeiORCID,Lyu Xuchao,Markhard Andrew L.,Fu Sipei,Mardjuki Rachel E.,Cavanagh Peter E.,Zeng Xianfeng,Rajniak Jakub,Lu Nannan,Xiao Shuke,Zhao Meng,Dolores Moya-Garzon Maria,Truong Steven D.,Chou Jonathan Chiu-Chun,Wat Lianna W.,Chidambaranathan-Reghupaty Saranya,Coassolo Laetitia,Xu Duo,Shen Fangfang,Huang Wentao,Ramirez Cuauhtemoc B.,Jang Cholsoon,Svensson Katrin J.ORCID,Fischbach Michael AORCID,Long Jonathan Z.

Abstract

SummaryTaurine is a conditionally essential micronutrient and one of the most abundant amino acids in humans1–3. In endogenous taurine metabolism, dedicated enzymes are involved in biosynthesis of taurine from cysteine as well as the downstream derivatization of taurine into secondary taurine metabolites4,5. One such taurine metabolite is N-acetyltaurine6. Levels of N-acetyltaurine are dynamically regulated by diverse physiologic perturbations that alter taurine and/or acetate flux, including endurance exercise7, nutritional taurine supplementation8, and alcohol consumption6,9. While taurine N-acetyltransferase activity has been previously detected in mammalian cells6,7, the molecular identity of this enzyme, and the physiologic relevance of N-acetyltaurine, have remained unknown. Here we show that the orphan body mass index-associated enzyme PTER (phosphotriesterase-related)10is the principal mammalian taurine N-acetyltransferase/hydrolase. In vitro, recombinant PTER catalyzes bidirectional taurine N-acetylation with free acetate as well as the reverse N-acetyltaurine hydrolysis reaction. Genetic ablation of PTER in mice results in complete loss of tissue taurine N-acetyltransferase/hydrolysis activities and systemic elevation of N-acetyltaurine levels. Upon stimuli that increase taurine levels, PTER-KO mice exhibit lower body weight, reduced adiposity, and improved glucose homeostasis. These phenotypes are recapitulated by administration of N-acetyltaurine to wild-type mice. Lastly, the anorexigenic and anti-obesity effects of N-acetyltaurine require functional GFRAL receptors. Together, these data uncover enzymatic control of a previously enigmatic pathway of secondary taurine metabolism linked to energy balance.

Publisher

Cold Spring Harbor Laboratory

Reference37 articles.

1. Taurine: a conditionally essential amino acid in humans? An overview in health and disease;Nutr Hosp,2002

2. Review: taurine: a “very essential” amino acid;Mol Vis,2012

3. Physiological role of taurine - from organism to organelle

4. Metabolism of Sulfur-Containing Amino Acids

5. Biochemistry and physiology of taurine and taurine derivatives.

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