间充质干细胞移植治疗的新视角:针对铁下垂途径。

Yuzhu Xu, Pan Fan, Lei Liu, X U Xuanfei, Lele Zhang, Jiadong Wang, Yuao Tao, Xiaolong Li, Xi Li, Yuntao Wang
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引用次数: 0

摘要

体外培养扩增的间充质干细胞(MSCs)因其具有愈合组织损伤的能力而受到广泛的研究。间充质干细胞移植是促进受损组织的修复和丢失细胞的替换或保护存活细胞的有效方法,但目前间充质干细胞移植的效率受到移植后短时间内间充质干细胞大量丢失的限制。因此,迫切需要提高骨髓间充质干细胞治疗疗效的策略。铁超载、活性氧沉积和抗氧化能力下降抑制间充质干细胞的增殖和再生,从而加速细胞死亡。值得注意的是,铁超载引起的氧化应激(OS)和抗氧化防御不足可导致铁下垂。上睑下垂可能会抑制间充质干细胞移植后的细胞存活,从而降低临床疗效。在这篇综述中,我们探讨了铁下垂在MSC性能中的作用。由于对移植MSCs中铁下垂的研究较少,因此迫切需要进一步的研究来增强MSCs的体内植入、功能和持续时间。
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Novel perspective in transplantation therapy of mesenchymal stem cells: targeting the ferroptosis pathway.

Ex vivo culture-amplified mesenchymal stem cells (MSCs) have been studied because of their capacity for healing tissue injury. MSC transplantation is a valid approach for promoting the repair of damaged tissues and replacement of lost cells or to safeguard surviving cells, but currently the efficiency of MSC transplantation is constrained by the extensive loss of MSCs during the short post-transplantation period. Hence, strategies to increase the efficacy of MSC treatment are urgently needed. Iron overload, reactive oxygen species deposition, and decreased antioxidant capacity suppress the proliferation and regeneration of MSCs, thereby hastening cell death. Notably, oxidative stress (OS) and deficient antioxidant defense induced by iron overload can result in ferroptosis. Ferroptosis may inhibit cell survival after MSC transplantation, thereby reducing clinical efficacy. In this review, we explore the role of ferroptosis in MSC performance. Given that little research has focused on ferroptosis in transplanted MSCs, further study is urgently needed to enhance the in vivo implantation, function, and duration of MSCs.

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