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骨髓、脂肪组织和皮肤来源的人基质(间质)干细胞在分子表型和分化潜能上存在差异。

Human stromal (mesenchymal) stem cells from bone marrow, adipose tissue and skin exhibit differences in molecular phenotype and differentiation potential.

机构信息

Stem Cell Unit, Department of Anatomy 28, College of Medicine, King Saud University, P.O. Box 2925, Riyadh, 11461, Kingdom of Saudi Arabia.

出版信息

Stem Cell Rev Rep. 2013 Feb;9(1):32-43. doi: 10.1007/s12015-012-9365-8.

Abstract

Human stromal (mesenchymal) stem cells (hMSCs) are multipotent stem cells with ability to differentiate into mesoderm-type cells e.g. osteoblasts and adipocytes and thus they are being introduced into clinical trials for tissue regeneration. Traditionally, hMSCs have been isolated from bone marrow, but the number of cells obtained is limited. Here, we compared the MSC-like cell populations, obtained from alternative sources for MSC: adipose tissue and skin, with the standard phenotype of human bone marrow MSC (BM-MSCs). MSC from human adipose tissue (human adipose stromal cells (hATSCs)) and human skin (human adult skin stromal cells, (hASSCs) and human new-born skin stromal cells (hNSSCs)) grew readily in culture and the growth rate was highest in hNSSCs and lowest in hATSCs. Compared with phenotype of hBM-MSC, all cell populations were CD34(-), CD45(-), CD14(-), CD31(-), HLA-DR(-), CD13(+), CD29(+), CD44(+), CD73(+), CD90(+),and CD105(+). When exposed to in vitro differentiation, hATSCs, hASSCs and hNSSCs exhibited quantitative differences in their ability to differentiate into adipocytes and to osteoblastic cells. Using a microarray-based approach we have unveiled a common MSC molecular signature composed of 33 CD markers including known MSC markers and several novel markers e.g. CD165, CD276, and CD82. However, significant differences in the molecular phenotype between these different stromal cell populations were observed suggesting ontological and functional differences. In conclusion, MSC populations obtained from different tissues exhibit significant differences in their proliferation, differentiation and molecular phenotype, which should be taken into consideration when planning their use in clinical protocols.

摘要

人基质(间质)干细胞(hMSCs)是多能干细胞,能够分化为中胚层类型的细胞,例如成骨细胞和脂肪细胞,因此它们被引入临床试验用于组织再生。传统上,hMSCs 是从骨髓中分离出来的,但获得的细胞数量有限。在这里,我们比较了从替代来源(脂肪组织和皮肤)获得的类似于 MSC 的细胞群体与标准人骨髓 MSC(BM-MSCs)表型。人脂肪组织(人脂肪基质细胞(hATSCs))和人皮肤(人成年皮肤基质细胞(hASSCs)和人新生儿皮肤基质细胞(hNSSCs))中的 MSC 很容易在培养中生长,其中 hNSSCs 的生长速度最快,而 hATSCs 的生长速度最慢。与 hBM-MSC 的表型相比,所有细胞群体均为 CD34(-)、CD45(-)、CD14(-)、CD31(-)、HLA-DR(-)、CD13(+)、CD29(+)、CD44(+)、CD73(+)、CD90(+)和 CD105(+)。当暴露于体外分化时,hATSCs、hASSCs 和 hNSSCs 在其分化为脂肪细胞和成骨细胞的能力方面表现出定量差异。使用基于微阵列的方法,我们揭示了一个由 33 个 CD 标记物组成的常见 MSC 分子特征,包括已知的 MSC 标记物和几个新的标记物,例如 CD165、CD276 和 CD82。然而,观察到这些不同基质细胞群体之间的分子表型存在显著差异,表明存在本体论和功能差异。总之,从不同组织中获得的 MSC 群体在增殖、分化和分子表型方面存在显著差异,在计划将其用于临床方案时应考虑这些差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dbaf/3563956/50ecc745ca92/12015_2012_9365_Fig1_HTML.jpg

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