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Senescence in Human Mesenchymal Stem Cells: Functional Changes and Implications in Stem Cell-Based Therapy

机译:人间充质干细胞的衰老:基于干细胞的疗法的功能变化和意义。

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摘要

Regenerative medicine is extensively interested in developing cell therapies using mesenchymal stem cells (MSCs), with applications to several aging-associated diseases. For successful therapies, a substantial number of cells are needed, requiring extensive ex vivo cell expansion. However, MSC proliferation is limited and it is quite likely that long-term culture evokes continuous changes in MSCs. Therefore, a substantial proportion of cells may undergo senescence. In the present review, we will first present the phenotypic characterization of senescent human MSCs (hMSCs) and their possible consequent functional alterations. The accumulation of oxidative stress and dysregulation of key differentiation regulatory factors determine decreased differentiation potential of senescent hMSCs. Senescent hMSCs also show a marked impairment in their migratory and homing ability. Finally, many factors present in the secretome of senescent hMSCs are able to exacerbate the inflammatory response at a systemic level, decreasing the immune modulation activity of hMSCs and promoting either proliferation or migration of cancer cells. Considering the deleterious effects that these changes could evoke, it would appear of primary importance to monitor the occurrence of senescent phenotype in clinically expanded hMSCs and to evaluate possible ways to prevent in vitro MSC senescence. An updated critical presentation of the possible strategies for in vitro senescence monitoring and prevention constitutes the second part of this review. Understanding the mechanisms that drive toward hMSC growth arrest and evaluating how to counteract these for preserving a functional stem cell pool is of fundamental importance for the development of efficient cell-based therapeutic approaches.
机译:再生医学对使用间充质干细胞(MSC)进行细胞疗法的开发具有广泛的兴趣,并将其应用于多种衰老相关疾病。为了成功的治疗,需要大量的细胞,需要大量的离体细胞扩增。但是,MSC的增殖受到限制,长期培养很可能引起MSC的持续变化。因此,很大比例的细胞可能会衰老。在本综述中,我们将首先介绍衰老的人类MSC(hMSC)的表型特征及其可能的功能改变。氧化应激的积累和关键分化调控因子的失调决定了衰老的hMSCs分化潜能的降低。衰老的hMSCs还显示出其迁移和归巢能力明显受损。最后,衰老的hMSCs的分泌组中存在的许多因素能够在全身水平上加剧炎症反应,降低hMSCs的免疫调节活性并促进癌细胞的增殖或迁移。考虑到这些变化可能引起的有害影响,在临床上扩展的hMSC中监测衰老表型的发生并评估预防体外MSC衰老的可能方法显得尤为重要。本综述的第二部分是对体外衰老监测和预防的可能策略的最新重要描述。理解导致hMSC生长停滞的机制并评估如何抵消这些机制以保留功能性干细胞池对于开发有效的基于细胞的治疗方法至关重要。

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