International Journal of Molecular Sciences (Jul 2021)

Suppressing Pyroptosis Augments Post-Transplant Survival of Stem Cells and Cardiac Function Following Ischemic Injury

  • Chang Youn Lee,
  • Seahyoung Lee,
  • Seongtae Jeong,
  • Jiyun Lee,
  • Hyang-Hee Seo,
  • Sunhye Shin,
  • Jun-Hee Park,
  • Byeong-Wook Song,
  • Il-Kwon Kim,
  • Jung-Won Choi,
  • Sang Woo Kim,
  • Gyoonhee Han,
  • Soyeon Lim,
  • Ki-Chul Hwang

DOI
https://doi.org/10.3390/ijms22157946
Journal volume & issue
Vol. 22, no. 15
p. 7946

Abstract

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The acute demise of stem cells following transplantation significantly compromises the efficacy of stem cell-based cell therapeutics for infarcted hearts. As the stem cells transplanted into the damaged heart are readily exposed to the hostile environment, it can be assumed that the acute death of the transplanted stem cells is also inflicted by the same environmental cues that caused massive death of the host cardiac cells. Pyroptosis, a highly inflammatory form of programmed cell death, has been added to the list of important cell death mechanisms in the damaged heart. However, unlike the well-established cell death mechanisms such as necrosis or apoptosis, the exact role and significance of pyroptosis in the acute death of transplanted stem cells have not been explored in depth. In the present study, we found that M1 macrophages mediate the pyroptosis in the ischemia/reperfusion (I/R) injured hearts and identified miRNA-762 as an important regulator of interleukin 1β production and subsequent pyroptosis. Delivery of exogenous miRNA-762 prior to transplantation significantly increased the post-transplant survival of stem cells and also significantly ameliorated cardiac fibrosis and heart functions following I/R injury. Our data strongly suggest that suppressing pyroptosis can be an effective adjuvant strategy to enhance the efficacy of stem cell-based therapeutics for diseased hearts.

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