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微纤维结构掩盖了出生后组织中的原纤维蛋白-2。

Microfibril structure masks fibrillin-2 in postnatal tissues.

机构信息

Shriners Hospital for Children, 3101 SW Sam Jackson Park Rd., Portland, OR 97239, USA.

出版信息

J Biol Chem. 2010 Jun 25;285(26):20242-51. doi: 10.1074/jbc.M109.087031. Epub 2010 Apr 19.

Abstract

Fibrillin microfibrils are polymeric structures present in connective tissues. The importance of fibrillin microfibrils to connective tissue function has been demonstrated by the multiple genetic disorders caused by mutations in fibrillins and in microfibril-associated molecules. However, knowledge of microfibril structure is limited, largely due to their insolubility. Most previous studies have focused on how fibrillin-1 is organized within microfibril polymers. In this study, an immunochemical approach was used to circumvent the insolubility of microfibrils to determine the role of fibrillin-2 in postnatal microfibril structure. Results obtained from studies of wild type and fibrillin-1 null tissues, using monoclonal and polyclonal antibodies with defined epitopes, demonstrated that N-terminal fibrillin-2 epitopes are masked in postnatal microfibrils and can be revealed by enzymatic digestion or by genetic ablation of Fbn1. From these studies, we conclude that fetal fibrillin polymers form an inner core within postnatal microfibrils and that microfibril structure evolves as growth and development proceed into the postnatal period. Furthermore, documentation of a novel cryptic site present in EGF4 in fibrillin-1 underscores the molecular complexity and tissue-specific differences in microfibril structure.

摘要

原纤维微纤维是存在于结缔组织中的聚合结构。纤维结合蛋白和微纤维相关分子突变引起的多种遗传疾病证明了纤维微纤维对结缔组织功能的重要性。然而,由于其不溶性,对微纤维结构的了解有限。大多数先前的研究都集中在纤维结合蛋白-1如何在微纤维聚合物中组织。在这项研究中,采用免疫化学方法绕过微纤维的不溶性,以确定纤维结合蛋白-2在出生后微纤维结构中的作用。使用具有定义表位的单克隆和多克隆抗体对野生型和纤维结合蛋白-1 缺失组织进行的研究结果表明,N 端纤维结合蛋白-2 表位在出生后微纤维中被掩盖,可通过酶消化或 Fbn1 的遗传缺失来揭示。从这些研究中,我们得出结论,胎儿纤维结合蛋白聚合物在出生后的微纤维中形成一个内芯,并且微纤维结构随着生长和发育进入出生后时期而演变。此外,在纤维结合蛋白-1 中的 EGF4 中存在一个新的隐匿位点的证明强调了微纤维结构的分子复杂性和组织特异性差异。

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