Dysregulated bile acid signaling contributes to the neurological impairment in murine models of acute and chronic liver failure

BACKGROUND: Hepatic encephalopathy (HE), a severe neuropsychiatric complication, is associated with increased blood levels of ammonia and bile acids (BAs). We sought to determine (1) whether abnormally increased blood BAs in liver cirrhotic patients with HE is caused by elevation of apical sodium-de...

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Autores principales: Xie, Guoxiang, Wang, Xiaoning, Jiang, Runqiu, Zhao, Aihua, Yan, Jingyu, Zheng, Xiaojiao, Huang, Fengjie, Liu, Xinzhu, Panee, Jun, Rajani, Cynthia, Yao, Chun, Yu, Herbert, Jia, Weiping, Sun, Beicheng, Liu, Ping, Jia, Wei
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2018
Materias:
Research paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6284422/
https://www.ncbi.nlm.nih.gov/pubmed/30344125
http://dx.doi.org/10.1016/j.ebiom.2018.10.030
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author Xie, Guoxiang
Wang, Xiaoning
Jiang, Runqiu
Zhao, Aihua
Yan, Jingyu
Zheng, Xiaojiao
Huang, Fengjie
Liu, Xinzhu
Panee, Jun
Rajani, Cynthia
Yao, Chun
Yu, Herbert
Jia, Weiping
Sun, Beicheng
Liu, Ping
Jia, Wei
author_facet Xie, Guoxiang
Wang, Xiaoning
Jiang, Runqiu
Zhao, Aihua
Yan, Jingyu
Zheng, Xiaojiao
Huang, Fengjie
Liu, Xinzhu
Panee, Jun
Rajani, Cynthia
Yao, Chun
Yu, Herbert
Jia, Weiping
Sun, Beicheng
Liu, Ping
Jia, Wei
author_sort Xie, Guoxiang
collection PubMed
description BACKGROUND: Hepatic encephalopathy (HE), a severe neuropsychiatric complication, is associated with increased blood levels of ammonia and bile acids (BAs). We sought to determine (1) whether abnormally increased blood BAs in liver cirrhotic patients with HE is caused by elevation of apical sodium-dependent BA transporter (ASBT)-mediated BA reabsorption; and (2) whether increased BA reabsorption would exacerbate ammonia-induced brain injuries. METHODS: We quantitatively measured blood BA and ammonia levels in liver cirrhosis patients with or without HE and healthy controls. We characterized ASBT expression, BA profiles, and ammonia concentrations in a chronic liver disease (CLD) mouse model induced by streptozotocin-high fat diet (STZ-HFD) and an azoxymethane (AOM) - induced acute liver failure (ALF) mouse model. These two mouse models were treated with SC-435 (ASBT inhibitor) and budesonide (ASBT activator), respectively. FINDINGS: Blood concentrations of ammonia and conjugated BAs were substantially increased in cirrhotic patients with HE (n = 75) compared to cirrhotic patients without HE (n = 126). Pharmacological inhibition of the enterohepatic BA circulation using a luminal- restricted ASBT inhibitor, SC-435, in mice with AOM-induced ALF and STZ-HFD -induced CLD effectively reduced BA and ammonia concentrations in the blood and brain, and alleviated liver and brain damages. Budesonide treatment induced liver and brain damages in normal mice, and exacerbated these damages in AOM-treated mice. INTERPRETATION: ASBT mediated BA reabsorption increases intestinal luminal pH and facilitates conversion of intestinal ammonium to ammonia, leading to abnormally high levels of neurotoxic ammonia and cytotoxic BAs in the blood and brain. Inhibition of intestinal ASBT with SC-435 can effectively remove neurotoxic BAs and ammonia from the bloodstream and thus, mitigate liver and brain injuries resulting from liver failure.
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spelling pubmed-62844222018-12-13 Dysregulated bile acid signaling contributes to the neurological impairment in murine models of acute and chronic liver failure Xie, Guoxiang Wang, Xiaoning Jiang, Runqiu Zhao, Aihua Yan, Jingyu Zheng, Xiaojiao Huang, Fengjie Liu, Xinzhu Panee, Jun Rajani, Cynthia Yao, Chun Yu, Herbert Jia, Weiping Sun, Beicheng Liu, Ping Jia, Wei EBioMedicine Research paper BACKGROUND: Hepatic encephalopathy (HE), a severe neuropsychiatric complication, is associated with increased blood levels of ammonia and bile acids (BAs). We sought to determine (1) whether abnormally increased blood BAs in liver cirrhotic patients with HE is caused by elevation of apical sodium-dependent BA transporter (ASBT)-mediated BA reabsorption; and (2) whether increased BA reabsorption would exacerbate ammonia-induced brain injuries. METHODS: We quantitatively measured blood BA and ammonia levels in liver cirrhosis patients with or without HE and healthy controls. We characterized ASBT expression, BA profiles, and ammonia concentrations in a chronic liver disease (CLD) mouse model induced by streptozotocin-high fat diet (STZ-HFD) and an azoxymethane (AOM) - induced acute liver failure (ALF) mouse model. These two mouse models were treated with SC-435 (ASBT inhibitor) and budesonide (ASBT activator), respectively. FINDINGS: Blood concentrations of ammonia and conjugated BAs were substantially increased in cirrhotic patients with HE (n = 75) compared to cirrhotic patients without HE (n = 126). Pharmacological inhibition of the enterohepatic BA circulation using a luminal- restricted ASBT inhibitor, SC-435, in mice with AOM-induced ALF and STZ-HFD -induced CLD effectively reduced BA and ammonia concentrations in the blood and brain, and alleviated liver and brain damages. Budesonide treatment induced liver and brain damages in normal mice, and exacerbated these damages in AOM-treated mice. INTERPRETATION: ASBT mediated BA reabsorption increases intestinal luminal pH and facilitates conversion of intestinal ammonium to ammonia, leading to abnormally high levels of neurotoxic ammonia and cytotoxic BAs in the blood and brain. Inhibition of intestinal ASBT with SC-435 can effectively remove neurotoxic BAs and ammonia from the bloodstream and thus, mitigate liver and brain injuries resulting from liver failure. Elsevier 2018-10-19 /pmc/articles/PMC6284422/ /pubmed/30344125 http://dx.doi.org/10.1016/j.ebiom.2018.10.030 Text en © 2018 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research paper
Xie, Guoxiang
Wang, Xiaoning
Jiang, Runqiu
Zhao, Aihua
Yan, Jingyu
Zheng, Xiaojiao
Huang, Fengjie
Liu, Xinzhu
Panee, Jun
Rajani, Cynthia
Yao, Chun
Yu, Herbert
Jia, Weiping
Sun, Beicheng
Liu, Ping
Jia, Wei
Dysregulated bile acid signaling contributes to the neurological impairment in murine models of acute and chronic liver failure
title Dysregulated bile acid signaling contributes to the neurological impairment in murine models of acute and chronic liver failure
title_full Dysregulated bile acid signaling contributes to the neurological impairment in murine models of acute and chronic liver failure
title_fullStr Dysregulated bile acid signaling contributes to the neurological impairment in murine models of acute and chronic liver failure
title_full_unstemmed Dysregulated bile acid signaling contributes to the neurological impairment in murine models of acute and chronic liver failure
title_short Dysregulated bile acid signaling contributes to the neurological impairment in murine models of acute and chronic liver failure
title_sort dysregulated bile acid signaling contributes to the neurological impairment in murine models of acute and chronic liver failure
topic Research paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6284422/
https://www.ncbi.nlm.nih.gov/pubmed/30344125
http://dx.doi.org/10.1016/j.ebiom.2018.10.030
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