Issue 2, 2015

Effects of compound Ginkgo biloba on intestinal permeability in rats with alcohol-induced liver injury

Abstract

This study aimed to investigate the effects of Compound Ginkgo biloba (CGB) on alterations in intestinal permeability and inflammation caused by endotoxin in chronic alcohol-induced liver injury. CGB was prepared by Ginkgo biloba extract and Rosa roxburghii in a 1 : 1 proportion. Rats were divided into four groups: control, ethanol, high-dosage CGB (0.6 g kg−1 d−1) and low-dosage CGB (0.2 g kg−1 d−1) group. Rats in the control group ingested a Lieber–DeCarli control liquid diet, while rats in the ethanol and CGB-treated groups ingested a Lieber–DeCarli alcohol liquid diet for eight weeks. CGB was orally administered from the beginning of the third week until the end of the experiment. CGB was observed to significantly reduce the activities of serum ALT, AST, diamine oxidase (DAO) as well as levels of serum TG, D-lactic acid and plasma endotoxin in rats fed with Lieber–DeCarli ethanol liquid. Further, the hepatic steatosis was improved and the damage to intestinal tight junctions was also relieved effectively after CGB administration. Moreover, CGB significantly downregulated the expressions of TNF-α, lipopolysaccharide binding protein (LBP), CD14 and TLR4 in the liver and upregulated the expressions of tight junction proteins including ZO-1, occludin and claudin-1. In summary, this study demonstrated that CGB alleviated alcohol-induced liver injury and hepatic lipopolysaccharide signaling as well as gut barrier dysfunction through restoring tight junctions.

Graphical abstract: Effects of compound Ginkgo biloba on intestinal permeability in rats with alcohol-induced liver injury

Article information

Article type
Paper
Submitted
15 Aug 2014
Accepted
14 Nov 2014
First published
14 Nov 2014

Food Funct., 2015,6, 470-478

Effects of compound Ginkgo biloba on intestinal permeability in rats with alcohol-induced liver injury

H. Li, P. Qiu, J. Wang, C. Niu and S. Pan, Food Funct., 2015, 6, 470 DOI: 10.1039/C4FO00739E

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