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C/EBPβ调节角质形成细胞分化的早期事件,包括生长停滞以及角蛋白1和角蛋白10的表达。

C/EBPbeta modulates the early events of keratinocyte differentiation involving growth arrest and keratin 1 and keratin 10 expression.

作者信息

Zhu S, Oh H S, Shim M, Sterneck E, Johnson P F, Smart R C

机构信息

Molecular and Cellular Toxicology, Department of Toxicology, North Carolina State University, Raleigh, North Carolina 27695-7633, USA.

出版信息

Mol Cell Biol. 1999 Oct;19(10):7181-90. doi: 10.1128/MCB.19.10.7181.

Abstract

The epidermis is a stratified squamous epithelium composed primarily of keratinocytes that become postmitotic and undergo sequential changes in gene expression during terminal differentiation. The expression of the transcription factor CCAAT/enhancer binding protein beta (C/EBPbeta) within mouse epidermis and primary keratinocytes has recently been described; however, the function of C/EBPbeta within the epidermal keratinocyte is unknown. We report here that transient transfection of mouse primary keratinocytes with a C/EBP-responsive promoter-reporter construct resulted in a sevenfold increase in luciferase activity when keratinocytes were switched to culture conditions that induce growth arrest and differentiation. Forced expression of C/EBPbeta in BALB/MK2 keratinocytes inhibited growth, induced morphological changes consistent with a more differentiated phenotype, and upregulated two early markers of differentiation, keratin 1 (K1) and keratin 10 (K10) but had a minimal effect on the expression of late-stage markers, loricrin and involucrin. Analysis of the epidermis of C/EBPbeta-deficient mice revealed a mild epidermal hyperplasia and decreased expression of K1 and K10 but not of involucrin and loricrin. C/EBPbeta-deficient primary keratinocytes were partially resistant to calcium-induced growth arrest. Analysis of terminally differentiated spontaneously detached keratinocytes or those induced to differentiate by suspension culture revealed that C/EBPbeta-deficient keratinocytes displayed striking decreases in K1 and K10, while expression of later-stage markers was only minimally altered. Our results demonstrate that C/EBPbeta plays an important role in the early events of stratified squamous differentiation in keratinocytes involving growth arrest and K1 and K10 expression.

摘要

表皮是一种复层鳞状上皮,主要由角质形成细胞组成,这些角质形成细胞进入有丝分裂后期,并在终末分化过程中经历基因表达的一系列变化。最近已经描述了转录因子CCAAT/增强子结合蛋白β(C/EBPβ)在小鼠表皮和原代角质形成细胞中的表达;然而,C/EBPβ在表皮角质形成细胞中的功能尚不清楚。我们在此报告,当角质形成细胞转换为诱导生长停滞和分化的培养条件时,用C/EBP反应性启动子-报告基因构建体瞬时转染小鼠原代角质形成细胞会导致荧光素酶活性增加7倍。在BALB/MK2角质形成细胞中强制表达C/EBPβ可抑制生长,诱导与更分化表型一致的形态变化,并上调分化的两个早期标志物角蛋白1(K1)和角蛋白10(K10),但对晚期标志物兜甲蛋白和内披蛋白的表达影响最小。对C/EBPβ缺陷小鼠的表皮分析显示轻度表皮增生,K1和K10的表达降低,但兜甲蛋白和内披蛋白的表达未降低。C/EBPβ缺陷的原代角质形成细胞对钙诱导的生长停滞具有部分抗性。对终末分化的自发脱离的角质形成细胞或通过悬浮培养诱导分化的角质形成细胞的分析表明,C/EBPβ缺陷的角质形成细胞中K1和K10显著减少,而晚期标志物的表达仅略有改变。我们的结果表明,C/EBPβ在角质形成细胞分层鳞状分化的早期事件中起重要作用,涉及生长停滞以及K1和K10的表达。

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