Fructose Overconsumption Impairs Hepatic Manganese Homeostasis and Ammonia Disposal

Overview

Journal Nat Commun

Specialty Biology

Date 2023 Dec 1

PMID 38040719

Authors

Jian-Hui Shi

Yu-Xia Chen

Yingying Feng

Xiaohang Yang

Jie Lin

Ting Wang

Chun-Chun Wei

Xian-Hua Ma

Rui Yang

Dongmei Cao

Hai Zhang

Xiangyang Xie

Zhifang Xie

Weiping J Zhang

Affiliations

Soon will be listed here.

Abstract

Arginase, a manganese (Mn)-dependent enzyme, is indispensable for urea generation and ammonia disposal in the liver. The potential role of fructose in Mn and ammonia metabolism is undefined. Here we demonstrate that fructose overconsumption impairs hepatic Mn homeostasis and ammonia disposal in male mice. Fructose overexposure reduces liver Mn content as well as its activity of arginase and Mn-SOD, and impairs the clearance of blood ammonia under liver dysfunction. Mechanistically, fructose activates the Mn exporter Slc30a10 gene transcription in the liver in a ChREBP-dependent manner. Hepatic overexpression of Slc30a10 can mimic the effect of fructose on liver Mn content and ammonia disposal. Hepatocyte-specific deletion of Slc30a10 or ChREBP increases liver Mn contents and arginase activity, and abolishes their responsiveness to fructose. Collectively, our data establish a role of fructose in hepatic Mn and ammonia metabolism through ChREBP/Slc30a10 pathway, and postulate fructose dietary restriction for the prevention and treatment of hyperammonemia.

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