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Importance of Extracellular Matrix Protein 1 (ECM1) in Maintaining the Functional Integrity of the Human Skin

机译:细胞外基质蛋白1(ECM1)在维持人类皮肤功能完整性中的重要性

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The extracellular matrix protein 1 (ECM1) is an 85 kDa glycoprotein first identified in 1994. The threedimensional structure of ECM1 based on the third serum albumin domain was determined by in silico modelling in order to predict the most important binding site(s) of ECM1 with other protein partners in human skin. ECM1 consists of four domains: a first domain existing of α -helices (α D1), the serum albumin subdomain-like (SASDL) domain 2, the sequence homology comparable with the first subdomain of the third serum albumin domain, SASDL3 and SASDL4, resulting in four “finger-like” structures ideal for binding with different proteins. A role for ECM1 was proposed in endochondral bone formation, angiogenesis and skin differentiation. Increased evidence has emerged for a pivotal biological function of ECM1 in human skin; loss of function mutations in the ECM1 gene causes the autosomal recessive genodermatosis lipoid proteinosis and auto-antibodies against ECM1 in the auto-immune disease lichen sclerosus, sharing comparable skin pathology in the affected lesions. ECM1 is capable of binding variable skin structural and extracellular matrix molecules like perlecan, laminin 332, fibulin-1C/D, fibulin-3 and heparin, as well as dermal interstitial molecules like MMP-9, collagen type IV, fibronectin, hyaluronic acid and chondroitin sulphate. In this way, ECM1 could be one of the proteins capable of connecting the basolateral surface of the epidermis through the basement membrane to the underlying dermis, which suggest a role for ECM1 as "biological glue" in maintaining skin integrity and function.
机译:细胞外基质蛋白1(ECM1)是一种1994年首次鉴定的85 kDa糖蛋白。通过计算机模拟确定了基于第三个血清白蛋白结构域的ECM1的三维结构,以预测ECM1的最重要结合位点与人类皮肤中的其他蛋白质伴侣。 ECM1由四个域组成:存在α-螺旋(αD1)的第一个域,血清白蛋白亚域样(SASDL)域2,与第三血清白蛋白域的第一亚域SASDL3和SASDL4可比的序列同源性,产生四个“手指样”结构,非常适合与不同蛋白质结合。有人提出了ECM1在软骨内骨形成,血管生成和皮肤分化中的作用。关于人皮肤中ECM1的关键生物学功能的证据越来越多。 ECM1基因功能突变的缺失会导致常染色体隐性遗传性皮肤病,脂质样蛋白变性和自身免疫性疾病地衣硬化中针对ECM1的自身抗体,在受影响的病变中具有可比的皮肤病理学特征。 ECM1能够结合可变的皮肤结构和细胞外基质分子,例如perlecan,层粘连蛋白332,fibulin-1C / D,fibulin-3和肝素,以及皮肤间质分子,例如MMP-9,IV型胶原,纤连蛋白,透明质酸和硫酸软骨素。通过这种方式,ECM1可能是能够通过基底膜将表皮的基底外侧表面连接至底层真皮的蛋白质之一,这表明ECM1作为“生物胶”在维持皮肤完整性和功能方面的作用。

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