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Cripto-1 是人类胚胎癌细胞中致瘤性、未分化亚群的细胞表面标志物。

Cripto-1 is a cell surface marker for a tumorigenic, undifferentiated subpopulation in human embryonal carcinoma cells.

机构信息

Mammary Biology and Tumorigenesis Laboratory, Robert H. LurieCancer Center Northwestern University Feinberg School of Medicine, Chicago, Illinois, USA.

出版信息

Stem Cells. 2010 Aug;28(8):1303-14. doi: 10.1002/stem.463.

Abstract

Deregulation of stem cells is associated with the generation and progression of malignant tumors. In addition, genes that are associated with early embryogenesis are frequently expressed in cancer. Cripto-1 (CR-1), a glycosylphosphatidylinositol-linked glycoprotein, is expressed during early embryogenesis and in various human carcinomas. We demonstrated that human embryonal carcinoma (EC) cells are heterogeneous for CR-1 expression and consist of two distinct subpopulations: a CR-1(High) and a CR-1(Low) population. By segregating CR-1(High) and CR-1(Low) populations of NTERA2/D1 EC cells by fluorescence-activated cell sorting, we demonstrated that CR-1(High) cells were more tumorigenic than CR-1(Low) cells by an in vitro tumor sphere assay and by in vivo xenograft formation. The CR-1(High) population was enriched in mRNA expression for the pluripotent embryonic stem (ES) cell genes Oct4, Sox2, and Nanog. CR-1 expression in NTERA2/D1 cells was regulated by a Smad2/3-dependent autocrine loop, by the ES cell-related transcription factors Oct4/Nanog, and partially by the DNA methylation status of the promoter region. These results demonstrate that CR-1 expression is enriched in an undifferentiated, tumorigenic subpopulation and is regulated by key regulators of pluripotent stem cells.

摘要

干细胞的失调与恶性肿瘤的发生和发展有关。此外,与早期胚胎发生相关的基因经常在癌症中表达。CR-1(CR-1)是一种糖基磷脂酰肌醇连接的糖蛋白,在早期胚胎发生和各种人类癌中表达。我们证明人胚癌细胞(EC)在 CR-1 表达上是异质的,由两个不同的亚群组成:CR-1(高)和 CR-1(低)群体。通过荧光激活细胞分选分离 NTERA2/D1 EC 细胞的 CR-1(高)和 CR-1(低)群体,我们通过体外肿瘤球体测定和体内异种移植形成证明 CR-1(高)细胞比 CR-1(低)细胞具有更强的致瘤性。CR-1(高)群体富含多能胚胎干细胞(ES)基因 Oct4、Sox2 和 Nanog 的 mRNA 表达。NTERA2/D1 细胞中的 CR-1 表达受 Smad2/3 依赖性自分泌环、ES 细胞相关转录因子 Oct4/Nanog 以及启动子区域的 DNA 甲基化状态部分调节。这些结果表明,CR-1 表达在未分化的、致瘤性亚群中富集,并受多能干细胞的关键调节因子调节。

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