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Induced neural stem cell-derived astrocytes modulate complement activation and mediate neuroprotection following closed head injury

机译:闭合性颅脑损伤后,诱导的神经干细胞衍生星形胶质细胞调节补体激活并介导神经保护

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The complement system is a crucial component of immunity, and its activation has critical roles in neuroinflammatory response and cellular damage following closed head injury (CHI). We previously demonstrated that systemically injected induced neural stem cells (iNSCs) could modulate complement activation to ameliorate neuronal apoptosis in mouse CHI models. However, it remains unknown whether iNSC derivatives can regulate complement activation. In the present study, after CHI mouse serum treatment, we found dramatic decreases in the cellular viabilities of differentiated iNSCs. Interestingly, following CHI mouse serum treatment, the death of astrocytes derived from iNSCs which were pre-treated with CHI mouse serum was significantly decreased. Meanwhile, the deposition of C3 (C3d) and C5b-9 in these astrocytes was substantially reduced. Remarkably, we detected increased expression of complement receptor type 1-related protein y (Crry) in these astrocytes. Moreover, these astrocytes could reduce the numbers of apoptotic neurons via Crry expression post-CHI mouse serum treatment. Additionally, intracerebral-transplanted iNSCs, pre-treated with CHI mouse serum, significantly increased the levels of Crry expression in astrocytes to reduce the accumulation of C3d and C9 and the death of neurons in the brains of CHI mice. In summary, iNSCs receiving CHI mouse serum pre-treatment could enhance the expression of Crry in iNSC-derived astrocytes to modulate complement activation and mediate neuroprotection following CHI.
机译:补体系统是免疫的关键组成部分,其激活在闭合性颅脑损伤(CHI)后的神经炎症反应和细胞损伤中具有关键作用。我们以前证明,全身注射的诱导神经干细胞(iNSCs)可以调节补体激活,以改善小鼠CHI模型中的神经元凋亡。但是,iNSC衍生物是否可以调节补体激活仍然未知。在本研究中,CHI小鼠血清治疗后,我们发现分化的iNSCs的细胞活力急剧下降。有趣的是,在CHI小鼠血清处理后,使用CHI小鼠血清预处理的iNSC衍生的星形胶质细胞的死亡显着减少。同时,这些星形胶质细胞中C3(C3d)和C5b-9的沉积显着减少。值得注意的是,我们检测到这些星形胶质细胞中补体受体1型相关蛋白y(Crry)的表达增加。此外,这些星形胶质细胞可以通过CHI小鼠血清处理后的Crry表达减少凋亡神经元的数量。此外,经CHI小鼠血清预处理的脑内移植iNSCs显着增加了星形胶质细胞中Crry表达的水平,从而减少了CHI小鼠大脑中C3d和C9的积累以及神经元的死亡。总之,接受CHI小鼠血清预处理的iNSC可以增强iNSC衍生的星形胶质细胞中Crry的表达,从而调节CHI后的补体激活并介导神经保护作用。

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