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Pharmacological inhibition of mTOR attenuates replicative cell senescence and improves cellular function via regulating the STAT3-PIM1 axis in human cardiac progenitor cells
Ji Hye Park, Na Kyoung Lee, Hye Ji Lim, Seung Taek Ji, Yeon-Ju Kim, Woong Bi Jang, Da Yeon Kim, Songhwa Kang, Jisoo Yun, Jong Seong Ha, Hyungtae Kim, Dongjun Lee, Sang Hong Baek, Sang‐Mo Kwon
Experimental & Molecular Medicine · 2020 · ▲ 52 citations
Deregulated nutrient-sensing
Cellular senescence
Stem-cell exhaustion
Altered intercellular communication
Rapamycin / mTOR inhibition
Human
Mouse
Abstract
The mammalian target of mTOR(definition)-inhibiting drug studied for extending healthspan and lifespan." style="text-decoration:underline dotted; text-underline-offset:2px; cursor:help;">rapamycin(definition) (mTOR) signaling pathway efficiently regulates the energy state of cells and maintains tissue homeostasis. Dysregulation of the mTOR pathway has been implicated in several human diseases. Rapamycin is a specific inhibitor of mTOR and pharmacological inhibition of mTOR with rapamycin promote cardiac cell generation from the differentiation of mouse and human embryonic stem cells. These studies strongly implicate a role of sustained mTOR activity in the differentiating functions of embryonic stem cells; however, they do not directly address the required effect for sustained mTOR activity in human cardiac progenitor cells. In the present study, we evaluated the effect of mTOR inhibition by rapamycin on the cellular function of human cardiac progenitor cells and discovered that treatment with rapamycin markedly attenuated replicative cell senescence(definition) in human cardiac progenitor cells (hCPCs) and promoted their cellular functions. Furthermore, rapamycin not only inhibited mTOR signaling but also influenced signaling pathways, including STAT3 and PIM1, in hCPCs. Therefore, these data reveal a crucial function for rapamycin in senescent hCPCs and provide clinical strategies based on chronic mTOR activity.
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- 10.1038/s12276-020-0374-4
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- 2026-06-13 MST
Cite this
APA
Park, J.H., Lee, N.K., Lim, H.J., Ji, S.T., Kim, Y., Jang, W.B., Kim, D.Y., Kang, S., Yun, J., Ha, J.S., Kim, H., Lee, D., Baek, S.H., & Kwon, S. (2020). Pharmacological inhibition of mTOR attenuates replicative cell senescence and improves cellular function via regulating the STAT3-PIM1 axis in human cardiac progenitor cells. <em>Experimental & Molecular Medicine</em>. https://doi.org/10.1038/s12276-020-0374-4
Vancouver
Park JH, Lee NK, Lim HJ, Ji ST, Kim Y, Jang WB, et al. Pharmacological inhibition of mTOR attenuates replicative cell senescence and improves cellular function via regulating the STAT3-PIM1 axis in human cardiac progenitor cells. Experimental & Molecular Medicine. 2020. doi:10.1038/s12276-020-0374-4.
BibTeX
@article{ji2020Pharma,
title = {Pharmacological inhibition of mTOR attenuates replicative cell senescence and improves cellular function via regulating the STAT3-PIM1 axis in human cardiac progenitor cells},
author = {Ji Hye Park and Na Kyoung Lee and Hye Ji Lim and Seung Taek Ji and Yeon-Ju Kim and Woong Bi Jang and Da Yeon Kim and Songhwa Kang and Jisoo Yun and Jong Seong Ha and Hyungtae Kim and Dongjun Lee and Sang Hong Baek and Sang‐Mo Kwon},
journal = {Experimental & Molecular Medicine},
year = {2020},
doi = {10.1038/s12276-020-0374-4},
}
Research neighborhood
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