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去除白血病抑制因子后,多能小鼠胚胎干细胞中与染色质相关的蛋白质表达下调。

Chromatin-related proteins in pluripotent mouse embryonic stem cells are downregulated after removal of leukemia inhibitory factor.

作者信息

Kurisaki Akira, Hamazaki Tatsuo S, Okabayashi Koji, Iida Tetsuo, Nishine Tsutomu, Chonan Ritsu, Kido Hiroshi, Tsunasawa Susumu, Nishimura Osamu, Asashima Makoto, Sugino Hiromu

机构信息

The Institute for Enzyme Research, University of Tokushima, 3-18-15, Kuramoto, Tokushima 770-8503, Japan.

出版信息

Biochem Biophys Res Commun. 2005 Sep 30;335(3):667-75. doi: 10.1016/j.bbrc.2005.07.128.

Abstract

Embryonic stem (ES) cells have generated enormous interest due to their capacity to self-renew and the potential for growing many different cell types in vitro. Leukemia inhibitory factor (LIF), bone morphogenetic proteins, octamer-binding protein 3 or 4, and Nanog are important factors in the maintenance of pluripotency in mouse ES cells. However, the mechanisms by which these factors regulate the pluripotency remain poorly understood. To identify other proteins involved in this process, we did a proteomic analysis of mouse ES cells that were cultured in the presence or absence of LIF. More than 100 proteins were found to be involved specifically in either the differentiation process or the maintenance of undifferentiated state. Among these, chromatin-related proteins were identified as the major proteins in nuclear extracts of undifferentiated cells. Analysis with real-time RT-PCR revealed that enrichment of these proteins in pluripotent ES cells was regulated at the transcriptional levels. These results suggest that specific chromatin-related proteins may be involved in maintaining the unique properties of pluripotent ES cells.

摘要

胚胎干细胞(ES细胞)因其自我更新能力以及在体外培养多种不同细胞类型的潜力而引发了极大的关注。白血病抑制因子(LIF)、骨形态发生蛋白、八聚体结合蛋白3或4以及Nanog是维持小鼠ES细胞多能性的重要因子。然而,这些因子调控多能性的机制仍知之甚少。为了鉴定参与这一过程的其他蛋白质,我们对在有或无LIF的情况下培养的小鼠ES细胞进行了蛋白质组学分析。发现100多种蛋白质分别特异性地参与分化过程或未分化状态的维持。其中,染色质相关蛋白被鉴定为未分化细胞核提取物中的主要蛋白质。实时RT-PCR分析表明,这些蛋白质在多能性ES细胞中的富集在转录水平受到调控。这些结果表明,特定的染色质相关蛋白可能参与维持多能性ES细胞的独特特性。

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