Gut butyrate-producers confer post-infarction cardiac protection

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

doi:10.1038/s41467-023-43167-5

Gut butyrate-producers confer post-infarction cardiac protection

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

藥理學科暨藥理學研究所

研究成果: Article › 同行評審

20 引文斯高帕斯（Scopus）

摘要

The 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.

原文	English
文章編號	7249
期刊	Nature communications
卷	14
發行號	1
DOIs	https://doi.org/10.1038/s41467-023-43167-5
出版狀態	Published - 2023 12月

All Science Journal Classification (ASJC) codes

一般化學
一般生物化學，遺傳學和分子生物學
一般物理與天文學

UN SDG

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10.1038/s41467-023-43167-5

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Chen, H. C., Liu, Y. W., Chang, K. C., Wu, Y. W., Chen, Y. M., Chao, Y. K., You, M. Y., Lundy, D. J., Lin, C. J., Hsieh, M. L., Cheng, Y. C., Prajnamitra, R. P., Lin, P. J., Ruan, S. C., Chen, D. H. K., Shih, E. S. C., Chen, K. W., Chang, S. S., Chang, C. M. C., ... Hsieh, P. C. H. (2023). Gut butyrate-producers confer post-infarction cardiac protection. Nature communications, 14(1), 文章 7249. https://doi.org/10.1038/s41467-023-43167-5

@article{6862ee83f29b46f3bb5ec25a17431d89,

title = "Gut butyrate-producers confer post-infarction cardiac protection",

abstract = "The 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.",

author = "Chen, {Hung Chih} and Liu, {Yen Wen} and Chang, {Kuan Cheng} and Wu, {Yen Wen} and Chen, {Yi Ming} and Chao, {Yu Kai} and You, {Min Yi} and Lundy, {David J.} and Lin, {Chen Ju} and Hsieh, {Marvin L.} and Cheng, {Yu Che} and Prajnamitra, {Ray P.} and Lin, {Po Ju} and Ruan, {Shu Chian} and Chen, {David Hsin Kuang} and Shih, {Edward S.C.} and Chen, {Ke Wei} and Chang, {Shih Sheng} and Chang, {Cindy M.C.} and Riley Puntney and Moy, {Amy Wu} and Cheng, {Yuan Yuan} and Chien, {Hsin Yuan} and Lee, {Jia Jung} and Wu, {Deng Chyang} and Hwang, {Ming Jing} and Jennifer Coonen and Hacker, {Timothy A.} and Yen, {C. L.Eric} and Rey, {Federico E.} and Kamp, {Timothy J.} and Hsieh, {Patrick C.H.}",

note = "Publisher Copyright: {\textcopyright} 2023, The Author(s).",

year = "2023",

month = dec,

doi = "10.1038/s41467-023-43167-5",

language = "English",

volume = "14",

journal = "Nature communications",

issn = "2041-1723",

publisher = "Nature Publishing Group",

number = "1",

}

Chen, HC, Liu, YW, Chang, KC, Wu, YW, Chen, YM, Chao, YK, You, MY, Lundy, DJ, Lin, CJ, Hsieh, ML, Cheng, YC, Prajnamitra, RP, Lin, PJ, Ruan, SC, Chen, DHK, Shih, ESC, Chen, KW, Chang, SS, Chang, CMC, Puntney, R, Moy, AW, Cheng, YY, Chien, HY, Lee, JJ, Wu, DC, Hwang, MJ, Coonen, J, Hacker, TA, Yen, CLE, Rey, FE, Kamp, TJ & Hsieh, PCH 2023, 'Gut butyrate-producers confer post-infarction cardiac protection', Nature communications, 卷 14, 編號 1, 7249. https://doi.org/10.1038/s41467-023-43167-5

TY - JOUR

T1 - Gut butyrate-producers confer post-infarction cardiac protection

AU - Chen, Hung Chih

AU - Liu, Yen Wen

AU - Chang, Kuan Cheng

AU - Wu, Yen Wen

AU - Chen, Yi Ming

AU - Chao, Yu Kai

AU - You, Min Yi

AU - Lundy, David J.

AU - Lin, Chen Ju

AU - Hsieh, Marvin L.

AU - Cheng, Yu Che

AU - Prajnamitra, Ray P.

AU - Lin, Po Ju

AU - Ruan, Shu Chian

AU - Chen, David Hsin Kuang

AU - Shih, Edward S.C.

AU - Chen, Ke Wei

AU - Chang, Shih Sheng

AU - Chang, Cindy M.C.

AU - Puntney, Riley

AU - Moy, Amy Wu

AU - Cheng, Yuan Yuan

AU - Chien, Hsin Yuan

AU - Lee, Jia Jung

AU - Wu, Deng Chyang

AU - Hwang, Ming Jing

AU - Coonen, Jennifer

AU - Hacker, Timothy A.

AU - Yen, C. L.Eric

AU - Rey, Federico E.

AU - Kamp, Timothy J.

AU - Hsieh, Patrick C.H.

PY - 2023/12

Y1 - 2023/12

N2 - The 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.

AB - The 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.

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VL - 14

JO - Nature communications

JF - Nature communications

IS - 1

M1 - 7249

ER -

Gut butyrate-producers confer post-infarction cardiac protection

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