Metabolic reprogramming of the intestinal microbiome with functional bile acid changes underlie the development of NAFLD

Metabolic reprogramming of the intestinal microbiome with functional bile acid changes underlie the development of NAFLD

Background and Aims Bile acids are hepatic metabolites and have many properties considered to be relevant to the pathophysiology of NAFLD. Circulating levels of the intestinal microbiome‐modified bile acid deoxycholate are increased in cirrhosis. Approach and Results To further elucidate the role of...

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Veröffentlicht in:Hepatology (Baltimore, Md.) Md.), 2022-12, Vol.76 (6), p.1811-1824
Hauptverfasser: Smirnova, Ekaterina, Muthiah, Mark D., Narayan, Nicole, Siddiqui, Mohamad S., Puri, Puneet, Luketic, Velimir A., Contos, Melissa J., Idowu, Michael, Chuang, Jen‐Chieh, Billin, Andrew N., Huss, Ryan S., Myers, Robert P., Boyett, Sherry, Seneshaw, Mulugeta, Min, Hae‐Ki, Mirshahi, Faridodin, Sanyal, Arun J.
Format: Artikel
Sprache:eng
Schlagworte:
Acids
Antibacterial activity
Bile
Bile acids
Bile Acids and Salts - pharmacology
Cirrhosis
Clinical trials
Deoxycholic acid
Drug development
Fibrosis
Gastrointestinal Microbiome
Hepatology
Humans
Hydrolase
Intestinal microflora
Intestine
Liver Cirrhosis
Metabolomics
Microbiomes
Non-alcoholic Fatty Liver Disease - metabolism
Pathophysiology
Phenotypes
RNA, Ribosomal, 16S
rRNA 16S
Transcriptomics
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Zusammenfassung:Background and Aims Bile acids are hepatic metabolites and have many properties considered to be relevant to the pathophysiology of NAFLD. Circulating levels of the intestinal microbiome‐modified bile acid deoxycholate are increased in cirrhosis. Approach and Results To further elucidate the role of bile acids and intestinal microbiota linked to bile acids in progressively severe NAFLD, a multiomic study of feces including 16S rRNA sequencing, microbial transcriptomics and metabolomics was performed in a cohort with varying phenotypes of NAFLD. Several bile acids of microbial origin derived from deoxycholic acid (DCA) (glycodeoxycholate, 7‐ketodeoxycholic acid, dehydrocholic acid) increased with disease activity and fibrosis stage. These were linked to increased expression of microbial bile salt hydrolase, bile acid operon (BaiCD) and hydroxysteroid dehydrogenases (hdhA) required for DCA and downstream metabolite synthesis providing a mechanistic basis for altered bile acid profiles with disease progression. Bacteroidetes and several genera of Lachnospiraceae family containing DCA generating genes increased with increasing disease severity, whereas several potentially beneficial microbes sensitive to antibacterial effects of DCA e.g., Ruminococcaceae were decreased. The clinical relevance of these data was confirmed in an independent cohort enrolled in a clinical trial for NASH where at entry DCA and its conjugates were associated with advanced fibrosis. In patients treated with placebo, DCA declined in those with fibrosis regression and increased in those with fibrosis progression. DCA rose further in those with compensated cirrhosis when they experienced decompensation. Conclusions These findings demonstrate a role for bile acids and the bile acid dependent microbiome in the development and progression of NAFLD and set the stage to leverage these findings for NASH biomarker development and for therapeutics.
ISSN:0270-9139
1527-3350
DOI:10.1002/hep.32568