Literature DB >> 29871716

HNF4α Regulates CSAD to Couple Hepatic Taurine Production to Bile Acid Synthesis in Mice.

Yifeng Wang1, David Matye1, Nga Nguyen1, Yuxia Zhang1, Tiangang Li1.   

Abstract

Cysteine dioxygenase 1 (CDO1) converts cysteine to cysteine sulfinic acid, which can be further converted by cysteine sulfinic acid decarboxylase (CSAD) to hypotaurine for taurine production. This cysteine catabolic pathway plays a major role in regulating hepatic cysteine homeostasis. Furthermore, taurine is used for bile acid conjugation, which enhances bile acid solubility and physiological function in the gut. Recent studies show that this cysteine catabolic pathway is repressed by bile acid signaling, but the molecular mechanisms have not been fully elucidated. The mechanisms of bile acid and farnesoid X receptor (FXR) regulation of hepatic CSAD expression were studied in mice and hepatocytes. We showed that hepatocyte nuclear factor 4α (HNF4α) bound the mouse CSAD proximal promoter and induced CSAD transcription. FXR-induced small heterodimer partner (SHP) repressed mouse CSAD gene transcription via interacting with HNF4α as a repressor. Consistent with this model, cholic acid feeding, obeticholic acid administration, and liver HNF4α knockdown reduced hepatic CSAD expression, while liver SHP knockout and apical sodium-dependent bile acid transporter (ASBT) inhibitor treatment induced hepatic CSAD expression in mice. Furthermore, TNF-α also inhibited CSAD expression, which may be partially mediated by reduced HNF4α in mouse hepatocytes. In contrast, bile acids and GW4064 did not inhibit CSAD expression in human hepatocytes. This study identified mouse CSAD as a novel transcriptional target of HNF4α. Bile acids and cytokines repress hepatic CSAD, which closely couples taurine production to bile acid synthesis in mice. The species-specific regulation of CSAD reflects the differential preference of bile acid conjugation to glycine and taurine in humans and mice, respectively.

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Year:  2018        PMID: 29871716      PMCID: PMC6190117          DOI: 10.3727/105221618X15277685544442

Source DB:  PubMed          Journal:  Gene Expr        ISSN: 1052-2166


  48 in total

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2.  Fibroblast growth factor 15 functions as an enterohepatic signal to regulate bile acid homeostasis.

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3.  Overexpression of cholesterol 7α-hydroxylase promotes hepatic bile acid synthesis and secretion and maintains cholesterol homeostasis.

Authors:  Tiangang Li; Michelle Matozel; Shannon Boehme; Bo Kong; Lisa-Mari Nilsson; Grace Guo; Ewa Ellis; John Y L Chiang
Journal:  Hepatology       Date:  2011-02-11       Impact factor: 17.425

4.  Enzymes and metabolites of cysteine metabolism in nonhepatic tissues of rats show little response to changes in dietary protein or sulfur amino acid levels.

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5.  Bile acid-CoA ligase deficiency--a new inborn error of bile acid metabolism.

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6.  Glycine and taurine conjugation of bile acids by a single enzyme. Molecular cloning and expression of human liver bile acid CoA:amino acid N-acyltransferase.

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10.  Development of a novel cysteine sulfinic Acid decarboxylase knockout mouse: dietary taurine reduces neonatal mortality.

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  3 in total

Review 1.  Bile acid-based therapies for non-alcoholic steatohepatitis and alcoholic liver disease.

Authors:  Tiangang Li; John Y L Chiang
Journal:  Hepatobiliary Surg Nutr       Date:  2020-04       Impact factor: 7.293

2.  Fatty liver and alteration of the gut microbiome induced by diallyl disulfide.

Authors:  Yanhong Yang; Fei Yang; Miaoling Huang; Huijuan Wu; Changyuan Yang; Xinyue Zhang; Lanxiang Yang; Guibin Chen; Shuqi Li; Qianyu Wang; Shaomin Liu; Yanyan Liu; Yuting Lei; Zili Lei; Jiao Guo
Journal:  Int J Mol Med       Date:  2019-09-24       Impact factor: 4.101

Review 3.  Taurine as a Natural Antioxidant: From Direct Antioxidant Effects to Protective Action in Various Toxicological Models.

Authors:  Peter F Surai; Katie Earle-Payne; Michael T Kidd
Journal:  Antioxidants (Basel)       Date:  2021-11-24
  3 in total

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