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真皮-表皮交界区的超分子相互作用:锚定原纤维-胶原蛋白VII与带状胶原纤维紧密结合。

Supramolecular interactions in the dermo-epidermal junction zone: anchoring fibril-collagen VII tightly binds to banded collagen fibrils.

作者信息

Villone Daniela, Fritsch Anja, Koch Manuel, Bruckner-Tuderman Leena, Hansen Uwe, Bruckner Peter

机构信息

Institute for Physiological Chemistry and Pathobiochemistry, University Hospital of Münster, 48149 Münster, Germany.

出版信息

J Biol Chem. 2008 Sep 5;283(36):24506-13. doi: 10.1074/jbc.M802415200. Epub 2008 Jul 3.

Abstract

The dermis and the epidermis of normal human skin are functionally separated by a basement membrane but, together, form a stable structural continuum. Anchoring fibrils reinforce this connection by insertion into the basement membrane and by intercalation with banded collagen fibrils of the papillary dermis. Structural abnormalities in collagen VII, the major molecular constituent of anchoring fibrils, lead to a congenital skin fragility condition, dystrophic epidermolysis bullosa, associated with skin blistering. Here, we characterized the molecular basis of the interactions between anchoring fibrils and banded collagen fibrils. Suprastructural fragments of the dermo-epidermal junction zone were generated by mechanical disruption and by separation with magnetic Immunobeads. Anchoring fibrils were tightly attached to banded collagen fibrils. In vitro binding studies demonstrated that a von Willebrand factor A-like motif in collagen VII was essential for binding of anchoring fibrils to reconstituted collagen I fibrils. Since collagen I and VII molecules reportedly undergo only weak interactions, the attachment of anchoring fibrils to collagen fibrils depends on supramolecular organization of their constituents. This complex is stabilized in situ and resists dissociation by strong denaturants.

摘要

正常人类皮肤的真皮层和表皮层在功能上由基底膜分隔,但二者共同构成一个稳定的结构连续体。锚定原纤维通过插入基底膜以及与乳头层真皮的带状胶原纤维相互嵌合来加强这种连接。胶原VII是锚定原纤维的主要分子成分,其结构异常会导致一种先天性皮肤脆弱病症——营养不良性大疱性表皮松解症,该病症与皮肤水疱形成有关。在此,我们对锚定原纤维与带状胶原纤维之间相互作用的分子基础进行了表征。通过机械破坏和用磁性免疫珠分离,生成了真皮 - 表皮交界区的超微结构片段。锚定原纤维紧密附着于带状胶原纤维。体外结合研究表明,胶原VII中一个类血管性血友病因子A基序对于锚定原纤维与重组I型胶原纤维的结合至关重要。由于据报道I型和VII型胶原分子仅发生微弱相互作用,所以锚定原纤维与胶原纤维的附着取决于其成分的超分子组织。这种复合物在原位稳定,并且能抵抗强变性剂的解离作用。

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