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在人类恶性胶质瘤中鉴定出两种不同的间充质基质细胞群体。

Identification of two distinct mesenchymal stromal cell populations in human malignant glioma.

作者信息

Svensson Andreas, Ramos-Moreno Tania, Eberstål Sofia, Scheding Stefan, Bengzon Johan

机构信息

Lund Stem Cell Center, BMC B10, Lund University, Klinikgatan 26, 221 84, Lund, Sweden.

Department of Clinical Sciences, Division of Neurosurgery, Lund University, Box 117, 221 00, Lund, Sweden.

出版信息

J Neurooncol. 2017 Jan;131(2):245-254. doi: 10.1007/s11060-016-2302-y. Epub 2016 Oct 18.

Abstract

Gene profiling has revealed that malignant gliomas can be divided into four distinct molecular subtypes, where tumors with a mesenchymal gene expression are correlated with short survival. The present investigation was undertaken to clarify whether human malignant gliomas contain endogenous mesenchymal stromal cells (MSC), fulfilling consensus criteria defined by The International Society for Cellular Therapy, recruited from the host. We found that MSC-like cells can be isolated from primary human malignant gliomas. Two distinct MSC-like cell populations, differing in their expression of the CD90 surface marker, were discovered after cell sorting. RNA sequencing revealed further genetic differences between these two cell populations and MSC-like cells lacking CD90 produced higher amounts of VEGF and PGE compared to cells with the true MSC phenotype, implying that the CD90 MSC-like cells most probably are more active in tumor vascularization and immunosuppression than their CD90 counterpart. The results highlight the CD90 subpopulation as an important tumor component, however, its functional effects in glioma remains to be resolved. Using the protocols presented here, it will be possible to isolate, characterize and analyze brain tumor-derived MSC-like cells in more detail and to further test their functions in vitro and in in vivo xenograft models of glioma.

摘要

基因谱分析显示,恶性胶质瘤可分为四种不同的分子亚型,其中具有间充质基因表达的肿瘤与生存期短相关。本研究旨在阐明人类恶性胶质瘤是否含有内源性间充质基质细胞(MSC),这些细胞符合国际细胞治疗协会定义的共识标准,是从宿主中招募而来的。我们发现可以从原发性人类恶性胶质瘤中分离出类似MSC的细胞。细胞分选后发现了两个不同的类似MSC的细胞群体,它们在CD90表面标志物的表达上有所不同。RNA测序揭示了这两个细胞群体之间进一步的基因差异,与具有真正MSC表型的细胞相比,缺乏CD90的类似MSC的细胞产生了更多的VEGF和PGE,这意味着CD90类似MSC的细胞在肿瘤血管生成和免疫抑制方面可能比其CD90对应细胞更活跃。结果突出了CD90亚群作为肿瘤重要组成部分的地位,然而,其在胶质瘤中的功能作用仍有待解决。使用本文介绍的方案,将有可能更详细地分离、表征和分析脑肿瘤来源的类似MSC的细胞,并进一步在体外和胶质瘤体内异种移植模型中测试它们的功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a460/5306185/9f1d67243fc2/11060_2016_2302_Fig1_HTML.jpg

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