首页> 外文期刊>Journal of Dental Research: Official Publication of the International Association for Dental Research >KGF Enhances Oral Epithelial Adhesion and Rete Peg Elongation via Integrins
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KGF Enhances Oral Epithelial Adhesion and Rete Peg Elongation via Integrins

机译:KGF增强口腔上皮粘附,通过整合素重温栓伸长率

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Oral epithelial adhesion to the lamina propria underlies the physiologic function of the oral mucosa and contributes to resisting bacterial invasion, preventing body fluid loss, and maintaining routine chewing; thus, understanding the factors that positively influence oral epithelial adhesion is a research topic of great interest. Rete pegs contribute to oral epithelial adhesion by enlarging the contact areas, whereas integrins are the major molecules that mediate epithelial cell adhesion to the basement membrane. Keratinocyte growth factor (KGF) can promote both rete peg elongation in the skin and the expression of integrins in various cell types. Herein, we tested the effects of submucosal injection of KGF in the ventral surfaces of rat tongues on oral epithelial adhesion. The data confirmed that topical injection of KGF elevated the adhesive forces, elongated the rete pegs, and increased the abundance of integrins, KGF, and KGF receptor on the rat tongue ventral surface. However, HYD-1 (Lys-Ile-Lys-Met-Val-Ile-Ser-Trp-Lys-Gly), an integrin antagonist, inhibited the KGF-enhanced epithelial adhesion and rete peg elongation. Moreover, KGF promoted the expression of integrin subunits α6, β4, α3, and β1 in human immortalized oral epithelial cells in 2- and 3-dimensional culture systems. In vitro cell attachment assays demonstrated that HYD-1 inhibited the adhesion of human immortalized oral epithelial cells on Matrigel. Strikingly, the expression of integrins, KGF, and KGFR in human masticatory mucosae with longer rete pegs was more abundant than that in the lining mucosae with shorter rete pegs. In addition, rete peg lengths were positively correlated with the expression levels of integrins, KGF, and KGF receptor. These findings indicate that KGF strengthens oral epithelial adhesion and rete peg elongation via integrins.
机译:对椎板的口腔上皮粘附粘附下来是口腔粘膜的生理功能,有助于抵抗细菌侵袭,防止体液损失,维持常规咀嚼;因此,了解积极影响口腔上皮粘连的因素是极其兴趣的研究课题。 Rete PEG通过扩大接触区域有助于口腔上皮粘附,而整联蛋白是将上皮细胞粘附到基底膜的主要分子。角质形成细胞生长因子(KGF)可以在皮肤中促进重温栓伸长率和各种细胞类型中的整联蛋白的表达。在此,我们测试了在口腔上皮粘附对大鼠舌腹表面中KGF的粘膜注射率注射的影响。该数据证实,KGF的局部注射升高了粘合力,伸长了重温栓,并增加了大鼠舌腹表面上的整联蛋白,KGF和KGF受体的丰度。然而,Hyd-1(Lys-Ile-Lys-Met-Val-Ile-Ser-Ser-Trp-Lys-Gy),整联蛋白拮抗剂,抑制了KGF增强的上皮粘附并重温臂伸长率。此外,KGF促进了2-和三维培养系统中人造永生的口腔上皮细胞中的整联蛋白α6,β4,α3和β1的表达。体外细胞附着测定证明Hyd-1抑制了人在Matrigel上的人永生上皮细胞的粘附性。尖锐的是,用更长的重温粘膜的人咀嚼粘膜中整联蛋白,KGF和KGFR的表达比衬里粘膜中的含量更加丰富,具有较短的重温钉。此外,Rete PEG长度与整联蛋白,KGF和KGF受体的表达水平正相关。这些发现表明,KGF强化口腔上皮粘附,通过整联蛋白重温栓伸长率。

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