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首页> 外文OA文献 >Distinct functions for integrins alpha 3 beta 1 in focal adhesions and alpha 6 beta 4/bullous pemphigoid antigen in a new stable anchoring contact (SAC) of keratinocytes: relation to hemidesmosomes
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Distinct functions for integrins alpha 3 beta 1 in focal adhesions and alpha 6 beta 4/bullous pemphigoid antigen in a new stable anchoring contact (SAC) of keratinocytes: relation to hemidesmosomes

机译:在角质形成细胞的新的稳定锚定接触(SAC)中,整合蛋白α3 beta 1在粘着斑中的独特功能和α6 beta 4 /球状天疱疮抗原的独特功能:与半桥粒的关系

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Basal cells of stratified epidermis are anchored to the basement membrane zone (BMZ) of skin via hemidesmosomes. We previously identified integrin alpha 3 beta 1, in focal adhesions (FAs), of cultured human keratinocytes (HFKs) as a mediator of HFK adhesion to secreted BMZ-like extracellular matrix (ECM; Carter, W.G., E.A. Wayner, T.S. Bouchard, and P. Kaur. 1990. J. Cell Biol. 110: 1387-1404). Here, we have examined the relation of integrins alpha 6 beta 4 and alpha 3 beta 1, to bullous pemphigoid antigen (BPA), a component of hemidesmosomes. We conclude that alpha 6 beta 4 in HFKs localizes in a new stable anchoring contact (SAC) that cooperates with alpha 3 beta 1- FAs to mediate adhesion to ECM, based on the following. (a) Comparison of secreted ECM, with exogenous laminin, fibronectin and collagen identified ECM as the preferred ligand for HFK adhesion and spreading and for formation of both alpha 6 beta 4-SACs and alpha 3 beta 1-FAs. (b) Inhibition of HFK adhesion with combined anti-alpha 3 beta 1 (P1B5) and anti-alpha 6 beta 4 (GoH3) antibodies indicated that both receptors were functional in adhesion to ECM while alpha 3 beta 1 played a dominant role in spreading. (c) alpha 6 beta 4 colocalized with BPA in SACs that were proximal to but excluded from FAs. Both alpha 6 beta 4- SACs and alpha 3 beta 1-FAs were in contact with the adhesion surface as indicated by antibody exclusion and interference reflection microscopy. (d) In contrast to alpha 3 beta 1-FAs, alpha 6 beta 4-SACs were present only in nonmotile cells, not associated with stress fibers, and were relatively stable to detergents and urea, suggesting a nonmotile, or anchoring function for SACs and motility functions for alpha 3 beta 1-FAs. (e) alpha 6 beta 4 formed a detergent-insoluble complex with exogenous ECM in an affinity isolation procedure, confirming the ability of an unidentified ECM ligand to interact with alpha 6 beta 4. (f) We suggest that alpha 6 beta 4/BPA-SACs in culture restrict migration of HFKs on ECM while alpha 3 beta 1-FAs form dynamic adhesions in spreading and migrating cells. alpha 6 beta 4/BPA-SACs in culture bear functional and compositional similarities to hemidesmosomes in skin.
机译:分层表皮的基底细胞通过半脂质体固定在皮肤的基底膜区(BMZ)上。我们之前在培养的人角质形成细胞(HFK)的粘着斑(FA)中鉴定了整联蛋白alpha 3 beta 1,作为HFK对分泌的BMZ样细胞外基质(ECM; Carter,WG,EA Wayner,TS Bouchard,and P.Kaur.1990.J.Cell Biol.110:1387-1404)。在这里,我们检查了整联蛋白α6 beta 4和α3 beta 1与大疱性类天疱疮抗原(BPA)(半桥粒的组成部分)之间的关系。我们得出结论,基于以下原因,HFK中的alpha 6 beta 4定位在一个新的稳定锚定接触(SAC)中,该接触与alpha 3 beta 1-FA协同介导对ECM的粘附。 (a)将分泌的ECM与外源层粘连蛋白,纤连蛋白和胶原蛋白进行比较,发现ECM是HFK粘附和扩散以及形成α6β4-SAC和α3β1-FA的优选配体。 (b)用抗α3beta 1(P1B5)和抗α6beta 4(GoH3)抗体联合抑制HFK粘附表明,这两种受体均具有与ECM粘附的功能,而α3beta 1在传播中起主要作用。 (c)alpha 6 beta 4与BPA在SA邻近但不包含在FA中的SAC共定位。如抗体排除和干扰反射显微镜所示,α6 beta 4- SAC和α3 beta 1-FA均与粘附表面接触。 (d)与alpha 3 beta 1-FAs相比,alpha 6 beta 4-SAC仅存在于不运动的细胞中,与应力纤维无关,并且对去污剂和尿素相对稳定,表明SAC的不运动或锚定功能和运动功能的alpha 3 beta 1-FA。 (e)α6 beta 4在亲和力分离过程中与外源ECM形成了去污剂不溶性复合物,证实了未知的ECM配体与α6 beta 4相互作用的能力。(f)我们建议α6 beta 4 / BPA -培养物中的SAC限制了HFK在ECM上的迁移,而alpha 3 beta 1-FA在扩散和迁移细胞中形成动态粘附。培养物中的α6 beta 4 / BPA-SAC与皮肤中的半脂质体具有功能和组成上的相似性。

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