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Collagen fibrillogenesis: fibronectin, integrins, and minor collagens as organizers and nucleators

机译:胶原原纤维形成:纤连蛋白,整联蛋白和次要胶原作为组织器和成核剂

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摘要

Collagens are triple helical proteins that occur in the extracellular matrix (ECM) and at the cell–ECM interface. There are more than 30 collagens and collagen-related proteins but the most abundant are collagens I and II that exist as D-periodic (where D = 67 nm) fibrils. The fibrils are of broad biomedical importance and have central roles in embryogenesis, arthritis, tissue repair, fibrosis, tumor invasion, and cardiovascular disease. Collagens I and II spontaneously form fibrils in vitro, which shows that collagen fibrillogenesis is a selfassembly process. However, the situation in vivo is not that simple; collagen I-containing fibrils do not form in the absence of fibronectin, fibronectin-binding and collagen-binding integrins, and collagen V. Likewise, the thin collagen II-containing fibrils in cartilage do not form in the absence of collagen XI. Thus, in vivo, cellular mechanisms are in place to control what is otherwise a protein self-assembly process. This review puts forward a working hypothesis for how fibronectin and integrins (the organizers) determine the site of fibril assembly, and collagens V and XI (the nucleators) initiate collagen fibrillogenesis.
机译:胶原蛋白是三螺旋蛋白,存在于细胞外基质(ECM)和细胞-ECM界面中。胶原蛋白和胶原蛋白相关的蛋白质超过30种,但数量最多的是呈D周期(其中D = 67 nm)原纤维存在的I型和II型胶原。所述原纤维具有广泛的生物医学重要性,并且在胚胎发生,关节炎,组织修复,纤维化,肿瘤侵袭和心血管疾病中具有中心作用。胶原蛋白I和II在体外自发形成纤维,这表明胶原蛋白纤维形成是一个自组装过程。但是,体内情况并非如此简单。在没有纤连蛋白,纤连蛋白结合和胶原结合整联蛋白以及胶原蛋白V的情况下,不会形成含胶原I的原纤维。同样,在没有胶原蛋白XI的情况下,软骨中也不会形成含有胶原I的细纤维。因此,在体内,细胞机制就位以控制蛋白质自组装过程。这项审查提出了一个可行的假设,即纤连蛋白和整联蛋白(组织者)如何确定纤丝的组装位置,以及胶原蛋白V和XI(成核剂)如何引发胶原蛋白原纤维形成。

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