Literature DB >> 27932556

Orally Administered Berberine Modulates Hepatic Lipid Metabolism by Altering Microbial Bile Acid Metabolism and the Intestinal FXR Signaling Pathway.

Runbin Sun1, Na Yang1, Bo Kong1, Bei Cao1, Dong Feng1, Xiaoyi Yu1, Chun Ge1, Jingqiu Huang1, Jianliang Shen1, Pei Wang1, Siqi Feng1, Fei Fei1, Jiahua Guo1, Jun He1, Nan Aa1, Qiang Chen1, Yang Pan1, Justin D Schumacher1, Chung S Yang1, Grace L Guo1, Jiye Aa2, Guangji Wang2.   

Abstract

Previous studies suggest that the lipid-lowering effect of berberine (BBR) involves actions on the low-density lipoprotein receptor and the AMP-activated protein kinase signaling pathways. However, the implication of these mechanisms is unclear because of the low bioavailability of BBR. Because the main action site of BBR is the gut and intestinal farnesoid X receptor (FXR) plays a pivotal role in the regulation of lipid metabolism, we hypothesized that the effects of BBR on intestinal FXR signaling pathway might account for its pharmacological effectiveness. Using wild type (WT) and intestine-specific FXR knockout (FXRint-/-) mice, we found that BBR prevented the development of high-fat-diet-induced obesity and ameliorated triglyceride accumulation in livers of WT, but not FXRint-/- mice. BBR increased conjugated bile acids in serum and their excretion in feces. Furthermore, BBR inhibited bile salt hydrolase (BSH) activity in gut microbiota, and significantly increased the levels of tauro-conjugated bile acids, especially tauro-cholic acid(TCA), in the intestine. Both BBR and TCA treatment activated the intestinal FXR pathway and reduced the expression of fatty-acid translocase Cd36 in the liver. These results indicate that BBR may exert its lipid-lowering effect primarily in the gut by modulating the turnover of bile acids and subsequently the ileal FXR signaling pathway. In summary, we provide the first evidence to suggest a new mechanism of BBR action in the intestine that involves, sequentially, inhibiting BSH, elevating TCA, and activating FXR, which lead to the suppression of hepatic expression of Cd36 that results in reduced uptake of long-chain fatty acids in the liver.
Copyright © 2016 by The American Society for Pharmacology and Experimental Therapeutics.

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Year:  2016        PMID: 27932556      PMCID: PMC5267522          DOI: 10.1124/mol.116.106617

Source DB:  PubMed          Journal:  Mol Pharmacol        ISSN: 0026-895X            Impact factor:   4.436


  65 in total

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10.  Berberine Ameliorates Hepatic Steatosis and Suppresses Liver and Adipose Tissue Inflammation in Mice with Diet-induced Obesity.

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Journal:  Sci Rep       Date:  2016-03-03       Impact factor: 4.379

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  35 in total

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2.  The gut microbiota modulator berberine ameliorates collagen-induced arthritis in rats by facilitating the generation of butyrate and adjusting the intestinal hypoxia and nitrate supply.

Authors:  Mengfan Yue; Yu Tao; Yulai Fang; Xingpan Lian; Qin Zhang; Yufeng Xia; Zhifeng Wei; Yue Dai
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7.  Berberine ameliorates blockade of autophagic flux in the liver by regulating cholesterol metabolism and inhibiting COX2-prostaglandin synthesis.

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