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首页> 外文期刊>Stem cells translational medicine. >Commitment to Aerobic Glycolysis Sustains Immunosuppression of Human Mesenchymal Stem Cells
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Commitment to Aerobic Glycolysis Sustains Immunosuppression of Human Mesenchymal Stem Cells

机译:对有氧糖酵解的承诺维持人类间充质干细胞的免疫抑制。

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Human mesenchymal stem cells (hMSCs) promote endogenous tissue repair in part by coordinating multiple components of the host immune system in response to environmental stimuli. Recent studies have shown that hMSCs are metabolically heterogeneous and actively reconfigure metabolism to support the biochemical demands of tissue repair. However, how hMSCs regulate their energy metabolism to support their immunomodulatory properties is largely unknown. This study investigates hMSC metabolic reconfiguration during immune activation and provides evidence that the hMSC metabolic state significantly influences their immunomodulatory properties. Specifically, hMSC immune polarization by interferon‐gamma (IFN‐γ) treatment leads to remodeling of hMSC metabolic pathways toward glycolysis, which is required to sustain the secretion of immunosuppressive factors. IFN‐γ exposure also inhibited mitochondrial electron transport activity, and the accumulation of mitochondrial reactive oxygen species plays an important signaling role in this metabolic reconfiguration. The results also show that activation of the Akt/mTOR signaling pathway is required for metabolic reconfiguration during immune polarization and that interruption of these metabolic changes alters the immune response in IFN‐γ licensed hMSCs. The results demonstrate the potential of altering hMSC metabolism to enhance their immunomodulatory properties and therapeutic efficacy in various diseases.
机译:人间充质干细胞(hMSCs)部分通过响应环境刺激而协调宿主免疫系统的多种成分来促进内源性组织修复。最近的研究表明,hMSC在代谢上是异质的,并积极地重新配置新陈代谢,以支持组织修复的生化需求。然而,hMSC如何调节其能量代谢以支持其免疫调节特性尚不清楚。这项研究调查了免疫激活过程中的hMSC代谢重构,并提供了hMSC代谢状态显着影响其免疫调节特性的证据。具体而言,干扰素-γ(IFN-γ)处理的hMSC免疫极化导致hMSC代谢途径向糖酵解的重塑,这是维持免疫抑制因子分泌所必需的。 IFN-γ暴露也抑制了线粒体的电子转运活性,线粒体活性氧的积累在这种代谢重构中起着重要的信号作用。结果还表明,激活Akt / mTOR信号通路对于免疫极化过程中的代谢重构而言是必需的,而这些代谢变化的中断会改变IFN-γ许可的hMSCs的免疫应答。结果证明了改变hMSC代谢以增强其在各种疾病中的免疫调节特性和治疗功效的潜力。

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