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恢复老年人类间充质干细胞的数量和质量,用于自体细胞治疗。

Restoring the quantity and quality of elderly human mesenchymal stem cells for autologous cell-based therapies.

机构信息

Department of Comprehensive Dentistry, University of Texas Health Science Center at San Antonio, 7703 Floyd Curl Drive, San Antonio, TX, 78229-3900, USA.

Department of Biomedical Engineering, University of Texas at San Antonio, San Antonio, TX, 78249, USA.

出版信息

Stem Cell Res Ther. 2017 Oct 27;8(1):239. doi: 10.1186/s13287-017-0688-x.

Abstract

BACKGROUND

Degenerative diseases are a major public health concern for the aging population and mesenchymal stem cells (MSCs) have great potential for treating many of these diseases. However, the quantity and quality of MSCs declines with aging, limiting the potential efficacy of autologous MSCs for treating the elderly population.

METHODS

Human bone marrow (BM)-derived MSCs from young and elderly donors were obtained and characterized using standard cell surface marker criteria (CD73, CD90, CD105) as recommended by the International Society for Cellular Therapy (ISCT). The elderly MSC population was isolated into four subpopulations based on size and stage-specific embryonic antigen-4 (SSEA-4) expression using fluorescence-activated cell sorting (FACS), and subpopulations were compared to the unfractionated young and elderly MSCs using assays that evaluate MSC proliferation, quality, morphology, intracellular reactive oxygen species, β-galactosidase expression, and adenosine triphosphate (ATP) content.

RESULTS

The ISCT-recommended cell surface markers failed to detect any differences between young and elderly MSCs. Here, we report that elderly MSCs were larger in size and displayed substantially higher concentrations of intracellular reactive oxygen species and β-galactosidase expression and lower amounts of ATP and SSEA-4 expression. Based on these findings, cell size and SSEA-4 expression were used to separate the elderly MSCs into four subpopulations by FACS. The original populations (young and elderly MSCs), as well as the four subpopulations, were then characterized before and after culture on tissue culture plastic and BM-derived extracellular matrix (BM-ECM). The small SSEA-4-positive subpopulation representing ~ 8% of the original elderly MSC population exhibited a "youthful" phenotype that was similar to that of young MSCs. The biological activity of this elderly subpopulation was inhibited by senescence-associated factors produced by the unfractionated parent population. After these "youthful" cells were isolated and expanded (three passages) on a "young microenvironment" (i.e., BM-ECM produced by BM cells from young donors), the number of cells increased ≈ 17,000-fold to 3 × 10 cells and retained their "youthful" phenotype.

CONCLUSIONS

These results suggest that it is feasible to obtain large numbers of high-quality autologous MSCs from the elderly population and establish personal stem cell banks that will allow serial infusions of "rejuvenated" MSCs for treating age-related diseases.

摘要

背景

退行性疾病是老龄化人口的主要公共卫生关注点,间充质干细胞(MSCs)在治疗许多此类疾病方面具有巨大潜力。然而,随着年龄的增长,MSCs 的数量和质量下降,限制了自体 MSC 治疗老年人群的潜在疗效。

方法

从小龄和老龄供体中获得人骨髓(BM)来源的 MSCs,并使用国际细胞治疗学会(ISCT)推荐的标准细胞表面标志物标准(CD73、CD90、CD105)进行特征鉴定。使用荧光激活细胞分选(FACS)根据大小和阶段特异性胚胎抗原-4(SSEA-4)表达将老龄 MSC 群体分离成四个亚群,并通过评估 MSC 增殖、质量、形态、细胞内活性氧(ROS)、β-半乳糖苷酶表达和三磷酸腺苷(ATP)含量的测定,将亚群与未分馏的年轻和老龄 MSCs 进行比较。

结果

ISCT 推荐的细胞表面标志物未能检测到年轻和老龄 MSCs 之间的任何差异。在这里,我们报告说,老龄 MSCs 体积更大,细胞内 ROS 浓度和β-半乳糖苷酶表达显著升高,ATP 含量和 SSEA-4 表达降低。基于这些发现,使用细胞大小和 SSEA-4 表达通过 FACS 将老龄 MSCs 分离成四个亚群。原始群体(年轻和老龄 MSCs)以及四个亚群在组织培养塑料和 BM 衍生细胞外基质(BM-ECM)上培养前后进行了特征鉴定。原始老龄 MSC 群体中约 8%的小 SSEA-4 阳性亚群表现出类似于年轻 MSC 的“年轻”表型。该老龄亚群的生物活性受到未分馏亲本群体产生的衰老相关因子的抑制。在这些“年轻”细胞通过在“年轻微环境”(即从小龄供体的 BM 细胞产生的 BM-ECM)上分离和扩增(三个传代)后,细胞数量增加了约 17000 倍,达到 3×10 个细胞,并保持其“年轻”表型。

结论

这些结果表明,从小龄和老龄供体中获得大量高质量的自体 MSCs 并建立个人干细胞库,以允许连续输注“ rejuvenated ”MSC 治疗与年龄相关的疾病是可行的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b017/5658952/c87f4fed5162/13287_2017_688_Fig1_HTML.jpg

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