Skeletal muscle satellite cell-derived mesenchymal stem cells ameliorate acute alcohol-induced liver injury

Jae Sik Chung, Soonjae Hwang, Ju Eun Hong, Minjeong Jo, Ki Jong Rhee, Seongyup Kim, Pil Young Jung, Youngdae Yoon, Seong Hee Kang, Hoon Ryu, Moon Young Kim, Keum Seok Bae, Young Woo Eom

Research output: Contribution to journalArticlepeer-review

1 Citation (Scopus)

Abstract

Cultured human skeletal-muscle satellite cells have properties of mesenchymal stem cells (skeletal muscle satellite cell-derived mesenchymal stem cells, SkMSCs) and play anti-inflammatory roles by secreting prostaglandin E2 and hepatocyte growth factor (HGF). To evaluate the utility of SkMSCs in treating liver diseases, we determined whether SkMSCs could ameliorate acute liver and gut inflammation induced by binge ethanol administration. Binge drinking of ethanol led to weight loss in the body and spleen, liver inflammation and steatosis, and increased serum ALT and AST levels (markers of liver injury), along with increased IL-1β, TNF-α, and iNOS expression levels in mice. However, levels of these binge-drinking-induced indicators were reduced by a single intraperitoneal treatment of SkMSCs. Furthermore, levels of bacteria-derived lipopolysaccharide decreased in the livers and sera of ethanol-exposed mice after SkMSC administration. SkMSCs decreased the extent of tissue inflammation and reduced villus and crypt lengths in the small intestine after alcohol binge drinking. SkMSCs also reduced the leakage of blood albumin, an indicator of leaky gut, in the stool of ethanol-exposed mice. Alcohol-induced damage to human colonic Caco-2/tc7 cells was also alleviated by HGF. Therefore, a single treatment with SkMSCs can attenuate alcoholic liver damage by reducing inflammatory responses in the liver and gut, suggesting that SkMSCs could be used in cell therapy to treat alcoholic liver diseases.

Original languageEnglish
Pages (from-to)353-363
Number of pages11
JournalInternational Journal of Medical Sciences
Volume19
Issue number2
DOIs
Publication statusPublished - 2022

Bibliographical note

Funding Information:
This research was funded by the Basic Science Research Program through the National Research Foundation of Korea (2017R1D1A1A02019212 and 2017R1D1A1A02018088) and NRF-2017-Fostering Core Leaders of the Future Basic Science Program/Global Ph.D. Fellowship Program (2017H1A2A1045727).

Funding Information:
This research was funded by the Basic Science Research Program through the National Research Foundation of Korea (2017R1D1A1A02019212 and 2017R1D1A1A02018088) and NRF-2017-Fostering Core Leaders of the Future Basic Science

Publisher Copyright:
© The author(s).

All Science Journal Classification (ASJC) codes

  • Medicine(all)

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