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源自PC13胚胎癌细胞的分化细胞获得有限寿命。

Acquisition of a limited lifespan by differentiating cells derived from PC13 embryonal carcinoma cells.

作者信息

Rayner M J, Pulsford J A

出版信息

J Cell Sci. 1984 Dec;72:227-40. doi: 10.1242/jcs.72.1.227.

Abstract

Retinoic acid (RA) has previously been shown to induce the differentiation of mouse embryonal carcinoma (EC) cells to endoderm-like cells that have a slower rate of proliferation and are nontumorigenic. These cells also acquire the ability to respond to a range of exogenous growth factors. We have analysed the change in growth phenotype for PC13 EC cells using video recordings and autoradiography. We have shown that the endoderm-like cells have a longer cell cycle time than their undifferentiated counterparts (five cell divisions after exposure to RA the differentiated cells had a median cell cycle time of 1800 min compared to 800 min for control cells). The endoderm-like cells also have a progressively decreasing probability of dividing again and this indicates that the differentiation process is accompanied by the acquisition of a limited life-span. The characteristics of mortal cells are well documented, and the endoderm-like cells demonstrate the properties of such cells. In addition, we have confirmed the observation that epidermal growth factor (EGF) can stimulate the proliferation of the endoderm-like cells and have shown, using autoradiography, that 92% of these cells express EGF receptors. Using video recordings, we have demonstrated that the effect of EGF is to shorten the cell cycle of the differentiating cells. We have also shown that EGF can enhance the survival of the endoderm-like cells and thereby prolong their life-span. It is known that EGF and other growth factors can prolong the life-span of mortal cells derived from normal tissues, but we have demonstrated that EGF can have this effect on the differentiated derivatives of a tumour cell.

摘要

视黄酸(RA)此前已被证明可诱导小鼠胚胎癌细胞(EC)分化为内胚层样细胞,这些细胞增殖速度较慢且无致瘤性。这些细胞还获得了对一系列外源性生长因子作出反应的能力。我们使用视频记录和放射自显影分析了PC13 EC细胞生长表型的变化。我们发现,内胚层样细胞的细胞周期时间比未分化的对应细胞更长(暴露于RA后经过五次细胞分裂,分化细胞的中位细胞周期时间为1800分钟,而对照细胞为800分钟)。内胚层样细胞再次分裂的概率也逐渐降低,这表明分化过程伴随着有限寿命的获得。终末分化细胞的特征已有充分记录,内胚层样细胞表现出此类细胞的特性。此外,我们证实了表皮生长因子(EGF)可刺激内胚层样细胞增殖的观察结果,并通过放射自显影表明,这些细胞中有92%表达EGF受体。使用视频记录,我们证明了EGF的作用是缩短分化细胞的细胞周期。我们还表明,EGF可提高内胚层样细胞的存活率,从而延长其寿命。已知EGF和其他生长因子可延长源自正常组织的终末分化细胞的寿命,但我们证明了EGF对肿瘤细胞的分化衍生物也有这种作用。

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