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差异氧暴露通过 mTOR 信号调节间充质干细胞代谢和增殖。

Differential Oxygen Exposure Modulates Mesenchymal Stem Cell Metabolism and Proliferation through mTOR Signaling.

机构信息

CNC-Centre for Neuroscience and Cell Biology, CIBB-Centre for Innovative Biomedicine and Biotechnology, University of Coimbra, Azinhaga de Santa Comba, Polo 3, 3000-548 Coimbra, Portugal.

Department of Life Sciences, University of Coimbra, Calçada Martim de Freitas, 3000-456 Coimbra, Portugal.

出版信息

Int J Mol Sci. 2022 Mar 29;23(7):3749. doi: 10.3390/ijms23073749.

Abstract

Mesenchymal stem cells reside under precise hypoxic conditions that are paramount in determining cell fate and behavior (metabolism, proliferation, differentiation, etc.). In this work, we show that different oxygen tensions promote a distinct proliferative response and affect the biosynthetic demand and global metabolic profile of umbilical cord-mesenchymal stem cells (UC-MSCs). Using both gas-based strategies and CoCl2 as a substitute for the costly hypoxic chambers, we found that specific oxygen tensions influence the fate of UC-MSCs differently. While 5% O2 potentiates proliferation, stimulates biosynthetic pathways, and promotes a global hypermetabolic profile, exposure to <1% O2 contributes to a quiescent-like cell state that relies heavily on anaerobic glycolysis. We show that using CoCl2 as a hypoxia substitute of moderate hypoxia has distinct metabolic effects, when compared with gas-based strategies. The present study also highlights that, while severe hypoxia regulates global translation via mTORC1 modulation, its effects on survival-related mechanisms are mainly modulated through mTORC2. Therefore, the experimental conditions used in this study establish a robust and reliable hypoxia model for UC-MSCs, providing relevant insights into how stem cells are influenced by their physiological environment, and how different strategies of modulating hypoxia may influence experimental outcomes.

摘要

间充质干细胞存在于精确的低氧条件下,这对于决定细胞命运和行为(代谢、增殖、分化等)至关重要。在这项工作中,我们表明不同的氧张力会促进独特的增殖反应,并影响脐带间充质干细胞(UC-MSCs)的生物合成需求和整体代谢特征。我们使用基于气体的策略和 CoCl2 作为昂贵的低氧室替代品,发现特定的氧张力会以不同的方式影响 UC-MSCs 的命运。虽然 5%的 O2 会增强增殖、刺激生物合成途径并促进整体高代谢特征,但暴露于 <1%的 O2 会导致类似于静止的细胞状态,严重依赖于无氧糖酵解。我们表明,与基于气体的策略相比,使用 CoCl2 作为中度低氧的替代物会产生不同的代谢效应。本研究还强调,虽然严重的低氧通过 mTORC1 调节来调节整体翻译,但它对与生存相关的机制的影响主要通过 mTORC2 来调节。因此,本研究中使用的实验条件为 UC-MSCs 建立了一个强大而可靠的低氧模型,提供了有关干细胞如何受其生理环境影响以及不同调节低氧的策略如何影响实验结果的相关见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/54d9/8998189/e3f10c062fdb/ijms-23-03749-g001.jpg

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