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表皮生长因子受体是维持表皮肿瘤基底层增殖细胞群所必需的。

The epidermal growth factor receptor is required to maintain the proliferative population in the basal compartment of epidermal tumors.

作者信息

Hansen L A, Woodson R L, Holbus S, Strain K, Lo Y C, Yuspa S H

机构信息

Laboratory of Cellular Carcinogenesis and Tumor Promotion, National Cancer Institute, Bethesda, Maryland 20892, USA.

出版信息

Cancer Res. 2000 Jul 1;60(13):3328-32.

Abstract

Previous studies using keratinocytes from epidermal growth factor receptor (EGFR)-deficient mice revealed that the EGFR is not required for papilloma formation initiated by a mutant rasHa gene, although the tumors that develop are very small (A. A. Dlugosz et aL, Cancer Res., 57: 3180-3188, 1997). The current study used a combination of bromodeoxyuridine pulse-chase, proliferating cell nuclear antigen distribution, and differentiation marker analysis to reveal the following: (a) the EGFR was required to maintain the proliferative population in the basal cell compartment of papillomas; (b) in the absence of EGFR, cycling tumor cells migrated into the suprabasal compartment and initiated the differentiation program prematurely; and (c) these changes were associated with cell cycle arrest. Further analysis of v-rasHa-transformed EGFR-deficient keratinocytes in vitro indicated that such cells migrated more on and attached less to extracellular matrix components. Together, these studies reveal that an essential function for the EGFR pathway in squamous tumors is to maintain a proliferative pool of basal cells and prevent premature terminal differentiation.

摘要

以往利用来自表皮生长因子受体(EGFR)缺陷小鼠的角质形成细胞进行的研究表明,尽管所形成的肿瘤非常小,但由突变型rasHa基因引发的乳头状瘤形成并不需要EGFR(A. A. 德鲁戈斯等人,《癌症研究》,57: 3180 - 3188, 1997)。当前的研究采用了溴脱氧尿苷脉冲追踪、增殖细胞核抗原分布以及分化标志物分析相结合的方法,以揭示以下内容:(a)EGFR是维持乳头状瘤基底细胞区室中增殖群体所必需的;(b)在缺乏EGFR的情况下,循环肿瘤细胞迁移到基底上层区室并过早启动分化程序;(c)这些变化与细胞周期停滞有关。对体外v - rasHa转化的EGFR缺陷角质形成细胞的进一步分析表明,此类细胞在细胞外基质成分上迁移更多且附着更少。这些研究共同表明,EGFR途径在鳞状肿瘤中的一项重要功能是维持基底细胞的增殖池并防止过早的终末分化。

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