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表膜联蛋白对于皮肤屏障功能以及单层和复层上皮中角蛋白网络细胞结构的完整性而言并非必需。

Epiplakin is dispensable for skin barrier function and for integrity of keratin network cytoarchitecture in simple and stratified epithelia.

作者信息

Spazierer Daniel, Fuchs Peter, Reipert Siegfried, Fischer Irmgard, Schmuth Matthias, Lassmann Hans, Wiche Gerhard

机构信息

Department of Molecular Cell Biology, Max F. Perutz Laboratories, University of Vienna, Dr. Bohrgasse 9, A-1030 Vienna, Austria.

出版信息

Mol Cell Biol. 2006 Jan;26(2):559-68. doi: 10.1128/MCB.26.2.559-568.2006.

Abstract

Epiplakin, a giant epithelial protein of >700 kDa, belongs to the plakin family of cytolinker proteins. It represents an atypical family member, however, as it consists entirely of plakin repeat domains but lacks any of the other domains commonly shared by plakins. Hence, its putative function as a cytolinker protein remains to be shown. To investigate epiplakin's biological role, we generated epiplakin-deficient mice by gene targeting in embryonic stem cells. Epiplakin-deficient mice were viable and fertile, without developing any discernible phenotype. Ultrastructurally, their epidermis revealed no differences compared to wild-type littermates, and cornified envelopes isolated from skin showed no alterations in shape or stability. Furthermore, neither embryonal formation nor later function of the epithelial barrier was affected. In primary cultures of epiplakin-deficient keratinocytes, the organization of actin filaments, microtubules, and keratin networks was found to be normal. Similarly, no alterations in keratin network organization were observed in simple epithelia of small intestine and liver or in primary hepatocytes. We conclude that, despite epiplakin's abundant and highly specific expression in stratified and simple epithelia, its absence in mice does not lead to severe skin dysfunctions, nor has it detectable consequences for keratin filament organization and cytoarchitecture of cells.

摘要

表皮斑蛋白是一种分子量大于700 kDa的巨大上皮蛋白,属于细胞连接蛋白的斑蛋白家族。然而,它是一个非典型家族成员,因为它完全由斑蛋白重复结构域组成,但缺乏斑蛋白通常共有的任何其他结构域。因此,其作为细胞连接蛋白的假定功能仍有待证实。为了研究表皮斑蛋白的生物学作用,我们通过对胚胎干细胞进行基因靶向操作,培育出了表皮斑蛋白缺陷型小鼠。表皮斑蛋白缺陷型小鼠能够存活且可育,未出现任何可识别的表型。在超微结构上,与野生型同窝小鼠相比,它们的表皮没有差异,从皮肤分离出的角质包膜在形状或稳定性上也没有改变。此外,上皮屏障的胚胎形成和后期功能均未受到影响。在表皮斑蛋白缺陷型角质形成细胞的原代培养中,发现肌动蛋白丝、微管和角蛋白网络的组织是正常的。同样,在小肠和肝脏的单层上皮或原代肝细胞中,也未观察到角蛋白网络组织的改变。我们得出结论,尽管表皮斑蛋白在复层和单层上皮中大量且高度特异性表达,但在小鼠中缺失它不会导致严重的皮肤功能障碍,对角蛋白丝组织和细胞的细胞结构也没有可检测到的影响。

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