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表皮分化调控的分子机制

Molecular aspects of control in epidermal differentiation.

作者信息

Vaughan F L, Bernstein I A

出版信息

Mol Cell Biochem. 1976 Sep 30;12(3):171-9. doi: 10.1007/BF01741715.

Abstract

The mammalian epidermis is organized into layers of structurally different cells--the basal, spinous, granular and cornified layers--which represent steps in the differentiative process that terminates in cornification and desquamation. Investigation of the molecular mechanisms that control this ordered sequence of events provides clues to the etiology of certain epidermal pathologies. DNA synthesis and mitosis are normally restricted to the basal layer. Several substances have been implicated in the mitotic control of epidermal cells, the loss of mitotic activity being the first major step in normal keratinization. Investigations performed in this laboratory indicate that isolated differentiated nuclei can replicate their DNA which they are inhibited from doing in situ. Addition of a high speed supernate from homogenized differentiated cells inhibited this synthetic activity in vitro suggesting the existence of a cytoplasmic inhibitor of DNA synthesis. It is not known whether mitotic inhibition in differentiated epidermal cells is a function of the inhibition of DNA replication. Contrary to previous assumptions, recent experimental evidence clearly indicates that, unlike DNA synthesis, RNA synthesis occurs in differentiated cells. Correlated with this synthetic activity is the observation that a protein rich in histidine is specifically formed in the granular cells. This protein appears to be a component of the keratohyalin granules which fill the cells of the granular layer. Investigations were conducted in this laboratory to determine whether control of the synthesis of this protein occurs at the level of translation or transcription. Translation, in vitro, of mRNA obtained from isolated populations of each epidermal cell type suggested that control of protein synthesis in the differentiating epidermis is transcriptional, i.e. only in the granular cell is there an mRNA for the histidine-rich protein. Transcription, in vitro, of chormatin isolated from the separated cell populations produced RNA with a ratio of cytidine to uracil consistent with the predicted mRNA for this protein thus providing additional support for the hypothesis that epidermal differentiation is controlled at the level of 'gene-readout'.

摘要

哺乳动物的表皮由结构不同的细胞层组成,即基底层、棘层、颗粒层和角质层,这些细胞层代表了以角质化和脱屑为终点的分化过程中的各个阶段。对控制这一有序事件序列的分子机制进行研究,可为某些表皮病变的病因提供线索。DNA合成和有丝分裂通常局限于基底层。有几种物质与表皮细胞的有丝分裂控制有关,有丝分裂活性的丧失是正常角质化的首要主要步骤。本实验室进行的研究表明,分离出的分化细胞核能够复制其DNA,而在原位它们却被抑制不能进行此过程。添加来自匀浆化分化细胞的高速上清液在体外抑制了这种合成活性,这表明存在一种DNA合成的细胞质抑制剂。尚不清楚分化的表皮细胞中的有丝分裂抑制是否是DNA复制抑制的一种功能。与先前的假设相反,最近的实验证据清楚地表明,与DNA合成不同,RNA合成发生在分化细胞中。与这种合成活性相关的是观察到在颗粒细胞中特异性形成了一种富含组氨酸的蛋白质。这种蛋白质似乎是填充颗粒层细胞的透明角质颗粒的一个组成部分。本实验室进行了研究,以确定这种蛋白质合成的控制是发生在翻译水平还是转录水平。对从每种表皮细胞类型的分离群体中获得的mRNA进行体外翻译表明,分化表皮中蛋白质合成的控制是转录性的,即只有在颗粒细胞中存在富含组氨酸蛋白质的mRNA。从分离的细胞群体中分离出的染色质进行体外转录,产生的RNA中胞嘧啶与尿嘧啶的比例与该蛋白质预测的mRNA一致,从而为表皮分化在“基因读出”水平受到控制这一假说提供了额外支持。

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