Gut butyrate-producers confer post-infarction cardiac protection

Author:

Chen Hung-Chih,Liu Yen-Wen,Chang Kuan-Cheng,Wu Yen-WenORCID,Chen Yi-Ming,Chao Yu-KaiORCID,You Min-Yi,Lundy David J.ORCID,Lin Chen-Ju,Hsieh Marvin L.,Cheng Yu-Che,Prajnamitra Ray P.,Lin Po-Ju,Ruan Shu-Chian,Chen David Hsin-KuangORCID,Shih Edward S. C.,Chen Ke-Wei,Chang Shih-Sheng,Chang Cindy M. C.,Puntney Riley,Moy Amy WuORCID,Cheng Yuan-Yuan,Chien Hsin-Yuan,Lee Jia-Jung,Wu Deng-Chyang,Hwang Ming-JingORCID,Coonen Jennifer,Hacker Timothy A.,Yen C-L. EricORCID,Rey Federico E.ORCID,Kamp Timothy J.ORCID,Hsieh Patrick C. H.ORCID

Abstract

AbstractThe gut microbiome and its metabolites are increasingly implicated in several cardiovascular diseases, but their role in human myocardial infarction (MI) injury responses have yet to be established. To address this, we examined stool samples from 77 ST-elevation MI (STEMI) patients using 16 S V3-V4 next-generation sequencing, metagenomics and machine learning. Our analysis identified an enriched population of butyrate-producing bacteria. These findings were then validated using a controlled ischemia/reperfusion model using eight nonhuman primates. To elucidate mechanisms, we inoculated gnotobiotic mice with these bacteria and found that they can produce beta-hydroxybutyrate, supporting cardiac function post-MI. This was further confirmed using HMGCS2-deficient mice which lack endogenous ketogenesis and have poor outcomes after MI. Inoculation increased plasma ketone levels and provided significant improvements in cardiac function post-MI. Together, this demonstrates a previously unknown role of gut butyrate-producers in the post-MI response.

Funder

Ministry of Science and Technology, Taiwan

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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