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首页> 外文期刊>Biochemical and Biophysical Research Communications >Potential role of 20S proteasome in maintaining stem cell integrity of human bone marrow stromal cells in prolonged culture expansion
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Potential role of 20S proteasome in maintaining stem cell integrity of human bone marrow stromal cells in prolonged culture expansion

机译:20S蛋白酶体在长期培养扩展中维持人骨髓基质细胞干细胞完整性的潜在作用

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摘要

Human bone marrow stromal cells (hBMSCs) could be used in clinics as precursors of multiple cell lineages following proper induction. Such application is impeded by their characteristically short lifespan, together with the increasing loss of proliferation capability and progressive reduction of differentiation potential after the prolonged culture expansion. In the current study, we addressed the possible role of 20S proteasomes in this process. Consistent with prior reports, long-term in vitro expansion of hBMSCs decreased cell proliferation and increased replicative senescence, accompanied by reduced activity and expression of the catalytic subunits PSMB5 and PSMB1, and the 20S proteasome overall. Application of the proteasome inhibitor MG132 produced a senescence-like phenotype in early passages, whereas treating late-passage cells with 18α-glycyrrhetinic acid (18α-GA), an agonist of 20S proteasomes, delayed the senescence progress, enhancing the proliferation and recovering the capability of differentiation. The data demonstrate that activation of 20S proteasomes assists in counteracting replicative senescence of hBMSCs expanded in vitro.
机译:人体骨髓基质细胞(hBMSC)可以在临床中用作经过适当诱导的多种细胞谱系的前体。由于其特征性的短寿命,以及延长的培养物扩增后增殖能力的丧失和分化潜能的逐渐降低,阻碍了这种应用。在当前的研究中,我们探讨了20S蛋白酶体在此过程中的可能作用。与先前的报道一致,hBMSC的长期体外扩增降低了细胞增殖和复制衰老,同时伴随着活性和催化亚基PSMB5和PSMB1以及整体20S蛋白酶体表达的降低。蛋白酶体抑制剂MG132的应用在早期传代中产生了衰老样表型,而用20S蛋白酶体的激动剂18α-甘草次酸(18α-GA)处理晚期传代细胞则延迟了衰老进程,增强了增殖并恢复了衰老。分化能力。数据表明20S蛋白酶体的激活有助于抵消体外扩增的hBMSCs的复制衰老。

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