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皮肤伤口愈合过程中角质形成细胞纤连蛋白受体功能的激活。

Activation of keratinocyte fibronectin receptor function during cutaneous wound healing.

作者信息

Grinnell F, Toda K, Takashima A

机构信息

Department of Cell Biology and Anatomy, University of Texas Health Science Center, Dallas 75235.

出版信息

J Cell Sci Suppl. 1987;8:199-209. doi: 10.1242/jcs.1987.supplement_8.11.

Abstract

Keratinocytes freshly isolated from unwounded skin could not attach and spread on fibronectin (FN)-coated culture dishes and could not bind and phagocytose FN-coated beads. These adhesive functions were activated, however, in keratinocytes that were isolated from healing wounds. Moreover, adhesiveness of basal keratinocytes to FN substrata was activated during epidermal cell or explant culture. Activation was specific for attachment to FN compared to other adhesion ligands, and occurred even when epidermal cells were cultured on collagen, basement membrane matrix, or lectin-coated substrata. Biochemical studies showed that keratinocytes have a 140 x 10(3) Mr FN receptor analogous to the fibroblast receptor for FN, and that this receptor is expressed in activated keratinocytes but not in keratinocytes freshly isolated from unwounded skin. The absence of FN receptors from keratinocytes in unwounded skin is not surprising since the basal keratinocytes of the epidermis are attached to a basement membrane containing laminin and type IV collagen. During wound repair, however, these cells migrate over or through a FN-coated matrix. Consequently, expression of FN receptors may be an essential feature of healing. Believing that FN is the required substratum for keratinocyte migration during wound healing, we have initiated clinical studies to determine if topical application of FN is useful as a therapy for non-healing cutaneous ulcers.

摘要

从未受伤皮肤中新鲜分离出的角质形成细胞无法在纤连蛋白(FN)包被的培养皿上附着和铺展,也无法结合和吞噬FN包被的珠子。然而,从愈合伤口中分离出的角质形成细胞的这些黏附功能被激活了。此外,在表皮细胞或外植体培养过程中,基底角质形成细胞对FN基质的黏附性也被激活。与其他黏附配体相比,这种激活对FN的附着具有特异性,即使表皮细胞在胶原蛋白、基底膜基质或凝集素包被的基质上培养时也会发生。生化研究表明,角质形成细胞有一种140×10³Mr的FN受体,类似于成纤维细胞的FN受体,并且这种受体在激活的角质形成细胞中表达,而在从未受伤皮肤中新鲜分离出的角质形成细胞中不表达。未受伤皮肤中的角质形成细胞缺乏FN受体并不奇怪,因为表皮的基底角质形成细胞附着于含有层粘连蛋白和IV型胶原蛋白的基底膜上。然而,在伤口修复过程中,这些细胞会在FN包被的基质上迁移或穿过。因此,FN受体的表达可能是愈合的一个基本特征。由于相信FN是伤口愈合过程中角质形成细胞迁移所需的基质,我们已经启动了临床研究,以确定局部应用FN是否对不愈合的皮肤溃疡有治疗作用。

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