Golden bile powder prevents drunkenness and alcohol-induced liver injury in mice via the gut microbiota and metabolic modulation

Yarong Wang; Zhenzhuang Zou; Sihua Wang; Airong Ren; Zhaolin Ding; Yingying Li; Yifang Wang; Zhengming Qian; Baolin Bian; Bo Huang; Guiwei Xu; Guozhen Cui

doi:10.1186/s13020-024-00912-2

Golden bile powder prevents drunkenness and alcohol-induced liver injury in mice via the gut microbiota and metabolic modulation

Chin Med. 2024 Mar 2;19(1):39. doi: 10.1186/s13020-024-00912-2.

Authors

Yarong Wang¹, Zhenzhuang Zou², Sihua Wang¹, Airong Ren¹, Zhaolin Ding¹, Yingying Li¹, Yifang Wang¹, Zhengming Qian³, Baolin Bian⁴, Bo Huang², Guiwei Xu¹, Guozhen Cui⁵

Affiliations

¹ School of Bioengineering, Zhuhai Campus of Zunyi Medical University, Zhuhai, 519000, Guangdong, China.
² Department of Pediatrics, The Fifth Affiliated Hospital of Zunyi Medical University, Zhuhai, 519000, Guangdong, China.
³ College of Medical Imaging Laboratory and Rehabilitation, Xiangnan University, Chenzhou, 423000, Hunan, China.
⁴ Institute of Chinese Materia Medica, China Academy of Chinese Medical Sciences, Beijing, 100700, China.
⁵ School of Bioengineering, Zhuhai Campus of Zunyi Medical University, Zhuhai, 519000, Guangdong, China. cgzum@hotmail.com.

Abstract

Background: Drunkenness and alcoholic liver disease (ALD) are critical public health issues associated with significant morbidity and mortality due to chronic overconsumption of alcohol. Traditional remedies, such as bear bile powder, have been historically acclaimed for their hepatoprotective properties. This study assessed the efficacy of a biotransformed bear bile powder known as golden bile powder (GBP) in alleviating alcohol-induced drunkenness and ALD.

Methods: A murine model was engineered to simulate alcohol drunkenness and acute hepatic injury through the administration of a 50% ethanol solution. Intervention with GBP and its effects on alcohol-related symptoms were scrutinized, by employing an integrative approach that encompasses serum metabolomics, network medicine, and gut microbiota profiling to elucidate the protective mechanisms of GBP.

Results: GBP administration significantly delayed the onset of drunkenness and decreased the duration of ethanol-induced inebriation in mice. Enhanced liver cell recovery was indicated by increased hepatic aldehyde dehydrogenase levels and superoxide dismutase activity, along with significant decreases in the serum alanine aminotransferase, aspartate aminotransferase, alkaline phosphatase, triglyceride, and total cholesterol levels (P < 0.05). These biochemical alterations suggest diminished hepatic damage and enhanced lipid homeostasis. Microbiota analysis via 16S rDNA sequencing revealed significant changes in gut microbial diversity and composition following alcohol exposure, and these changes were effectively reversed by GBP treatment. Metabolomic analyses demonstrated that GBP normalized the alcohol-induced perturbations in phospholipids, fatty acids, and bile acids. Correlation assessments linked distinct microbial genera to serum bile acid profiles, indicating that the protective efficacy of GBP may be attributable to modulatory effects on metabolism and the gut microbiota composition. Network medicine insights suggest the prominence of two active agents in GBP as critical for addressing drunkenness and ALD.

Conclusion: GBP is a potent intervention for alcohol-induced pathology and offers hepatoprotective benefits, at least in part, through the modulation of the gut microbiota and related metabolic cascades.

Keywords: Alcoholic liver disease; Drunkenness; Golden bile powder; Gut microbiota; Metabolomics; Network medicine.

Grants and funding

Qiankehe support [2023] General 071/Guizhou Province Science and Technology Program