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鉴定和描述腺病毒早期区域 1B 相关蛋白 5 作为未分化人胚胎干细胞表面标记物。

Identification and characterization of adenovirus early region 1B-associated protein 5 as a surface marker on undifferentiated human embryonic stem cells.

机构信息

Department of Bioscience and Biotechnology, Institute of Bioscience, Sejong University, Seoul, Korea.

出版信息

Stem Cells Dev. 2011 Apr;20(4):609-20. doi: 10.1089/scd.2010.0265. Epub 2011 Jan 16.

DOI:10.1089/scd.2010.0265
PMID:21083500
Abstract

Pluripotent human embryonic stem cells (hESCs) provide appropriate systems for developmental studies and prospective donor cell sources for regenerative medicine. Identification of surface markers specific to hESCs is a prerequisite for studying hESC biology and can be used to generate clinical-level donor cell preparations that are free from tumorigenic undifferentiated hESCs. We previously reported the generation of monoclonal antibodies that specifically recognize hESC surface antigens using a decoy immunization strategy. In this study, we show that monoclonal antibody 57-C11 recognizes a phosphorylated form of adenovirus early region 1B-associated protein 5 (E1B-AP5). E1B-AP5 is a nuclear RNA-binding protein, but we report that 57-C11-reactive E1B-AP5 is expressed on the surface of undifferentiated hESCs. In undifferentiated hESCs, 57-C11-reactive E1B-AP5 is localized to SSEA3-, SSEA4-, TRA-1-60-, TRA-1-81-, OCT4-, SOX2-, and NANOG-positive hESCs. In mixtures of undifferentiated hESCs and hESC-derived neurons, 57-C11 exclusively recognizes undifferentiated hESCs but not hESC-derived neuronal cells. Further, the expression of 57-C11-reactive E1B-AP5 decreases upon differentiation. Our results demonstrate that 57-C11-reactive E1B-AP5 is a novel surface molecule that is involved in the undifferentiated state of hESCs. As far as we know, this is the first report demonstrating that heterogeneous nuclear RNA-binding protein is expressed on the surface of undifferentiated hESCs.

摘要

多能人胚胎干细胞(hESCs)为发育研究提供了适当的系统,也是再生医学中潜在供体细胞的来源。鉴定 hESC 表面标志物是研究 hESC 生物学的前提条件,并且可以用于生成无致瘤性未分化 hESC 的临床级供体细胞制剂。我们之前报道了使用诱饵免疫策略生成特异性识别 hESC 表面抗原的单克隆抗体。在这项研究中,我们表明单克隆抗体 57-C11 识别腺病毒早期区域 1B 相关蛋白 5(E1B-AP5)的磷酸化形式。E1B-AP5 是一种核 RNA 结合蛋白,但我们报告称,57-C11 反应性 E1B-AP5 表达在未分化的 hESC 表面。在未分化的 hESC 中,57-C11 反应性 E1B-AP5 定位于 SSEA3、SSEA4、TRA-1-60、TRA-1-81、OCT4、SOX2 和 NANOG 阳性的 hESC。在未分化的 hESC 和 hESC 衍生神经元的混合物中,57-C11 仅识别未分化的 hESC,而不识别 hESC 衍生的神经元细胞。此外,分化后 57-C11 反应性 E1B-AP5 的表达减少。我们的结果表明,57-C11 反应性 E1B-AP5 是一种新型的表面分子,参与 hESC 的未分化状态。据我们所知,这是首次报道表明异质核 RNA 结合蛋白表达在未分化的 hESC 表面。

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