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球形体系列糖脂 SSEA-4 是体外和体内骨髓来源克隆多能基质细胞的标志物。

The globoseries glycosphingolipid SSEA-4 is a marker of bone marrow-derived clonal multipotent stromal cells in vitro and in vivo.

机构信息

Biologics and Genetic Therapies Directorate, Health Products and Food Branch , Health Canada, Ottawa, Canada.

出版信息

Stem Cells Dev. 2013 May 1;22(9):1387-97. doi: 10.1089/scd.2012.0547. Epub 2013 Jan 18.

Abstract

The therapeutic potential of multipotent stromal cells (MSC) may be enhanced by the identification of markers that allow their discrimination and enumeration both in vivo and in vitro. Here, we investigated the ability of embryonic stem cell-associated glycosphingolipids to isolate human MSC from both whole-bone-marrow (BM) and stromal cell cultures. Only SSEA-4 was consistently expressed on cells within the CD45loCD105hi marrow fraction and could be used to isolate cells with the capacity to give rise to stromal cultures containing MSC. Human stromal cultures, generated in either the presence or absence of serum, contained heterogeneous cell populations discriminated by the quantity of SSEA-4 epitopes detected on their surface. A low level of surface SSEA-4 (SSEA-4lo) correlated with undetectable levels of the α2,3-sialyltransferase-II enzyme required to synthesize SSEA-4; a reduced proliferative potential; and the loss of fat-, bone-, and cartilage-forming cells during long-term culture. In vitro, single cells with the capacity to generate multipotent stromal cultures were detected exclusively in the SSEA-4hi fraction. Our data demonstrate that a high level of surface epitopes for SSEA-4 provides a definitive marker of MSC from human BM.

摘要

多能基质细胞 (MSC) 的治疗潜力可以通过鉴定标记物来增强,这些标记物可以允许其在体内和体外进行区分和计数。在这里,我们研究了胚胎干细胞相关糖脂能够从整个骨髓 (BM) 和基质细胞培养物中分离人 MSC 的能力。只有 SSEA-4 在 CD45loCD105hi 骨髓部分的细胞中持续表达,并且可以用于分离具有产生包含 MSC 的基质培养物能力的细胞。在有或没有血清的情况下生成的人基质培养物包含通过其表面上检测到的 SSEA-4 表位的数量来区分的异质细胞群体。表面 SSEA-4 水平低 (SSEA-4lo) 与合成 SSEA-4 所需的 α2,3-唾液酸转移酶-II 酶的检测水平呈负相关;增殖潜力降低;并且在长期培养过程中脂肪、骨和软骨形成细胞丢失。在体外,具有生成多能基质培养物能力的单细胞仅在 SSEA-4hi 部分中检测到。我们的数据表明,表面 SSEA-4 表位的高水平提供了人 BM 中 MSC 的明确标记物。

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