Han, Ying-Hao; Mao, Ying-Ying; Lee, Kyung Ho; Cho, Hee Jun; Yu, Nan-Nan; Xing, Xiao-Ya; Wang, Ai-Guo; Jin, Mei-Hua; Hong, Kwan Soo; Sun, Hu-Nan; Kwon, Taeho

doi:10.1186/s12964-023-01331-w

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Title: Peroxiredoxin II regulates exosome secretion from dermal mesenchymal stem cells through the ISGylation signaling pathway.
Authors: Han, Ying-Hao; Mao, Ying-Ying; Lee, Kyung Ho; Cho, Hee Jun; Yu, Nan-Nan; Xing, Xiao-Ya; Wang, Ai-Guo; Jin, Mei-Hua; Hong, Kwan Soo; Sun, Hu-Nan; Kwon, Taeho
Abstract: Background: Exosomes are small extracellular vesicles that play important roles in intercellular communication and have potential therapeutic applications in regenerative medicine. Dermal mesenchymal stem cells (DMSCs) are a promising source of exosomes due to their regenerative and immunomodulatory properties. However, the molecular mechanisms regulating exosome secretion from DMSCs are not fully understood. Results: In this study, the role of peroxiredoxin II (Prx II) in regulating exosome secretion from DMSCs and the underlying molecular mechanisms were investigated. It was discovered that depletion of Prx II led to a significant reduction in exosome secretion from DMSCs and an increase in the number of intracellular multivesicular bodies (MVBs), which serve as precursors of exosomes. Mechanistically, Prx II regulates the ISGylation switch that controls MVB degradation and impairs exosome secretion. Specifically, Prx II depletion decreased JNK activity, reduced the expression of the transcription inhibitor Foxo1, and promoted miR-221 expression. Increased miR-221 expression inhibited the STAT signaling pathway, thus downregulating the expression of ISGylation-related genes involved in MVB degradation. Together, these results identify Prx II as a critical regulator of exosome secretion from DMSCs through the ISGylation signaling pathway. Conclusions: Our findings provide important insights into the molecular mechanisms regulating exosome secretion from DMSCs and highlight the critical role of Prx II in controlling the ISGylation switch that regulates DMSC-exosome secretion. This study has significant implications for developing new therapeutic strategies in regenerative medicine. -6AE1Qxi5fhihA5_M9L54L Video Abstract
Subjects: MESENCHYMAL stem cells; CELL communication; EXOSOMES; CELLULAR signal transduction; EXTRACELLULAR vesicles; SECRETION; REGENERATIVE medicine
Publication: Cell Communication & Signaling, 2023, Vol 21, Issue 1, p1
ISSN: 1478-811X
Publication type: Academic Journal
DOI: 10.1186/s12964-023-01331-w

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Peroxiredoxin II regulates exosome secretion from dermal mesenchymal stem cells through the ISGylation signaling pathway.

Han, Ying-Hao; Mao, Ying-Ying; Lee, Kyung Ho; Cho, Hee Jun; Yu, Nan-Nan; Xing, Xiao-Ya; Wang, Ai-Guo; Jin, Mei-Hua; Hong, Kwan Soo; Sun, Hu-Nan; Kwon, Taeho

MESENCHYMAL stem cells; CELL communication; EXOSOMES; CELLULAR signal transduction; EXTRACELLULAR vesicles; SECRETION; REGENERATIVE medicine

Cell Communication & Signaling, 2023, Vol 21, Issue 1, p1

1478-811X

Academic Journal

10.1186/s12964-023-01331-w