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胎球蛋白在血清诱导的胶原蛋白钙化中的重要作用。

The essential role of fetuin in the serum-induced calcification of collagen.

作者信息

Toroian Damon, Price Paul A

机构信息

Division of Biological Sciences, University of California, San Diego, La Jolla, CA 92093-0368, USA.

出版信息

Calcif Tissue Int. 2008 Feb;82(2):116-26. doi: 10.1007/s00223-007-9085-2. Epub 2007 Dec 21.

Abstract

The mineral in bone is located primarily within the collagen fibril, and during mineralization the fibril is formed first and then water within the fibril is replaced with mineral. Our goal is to understand the mechanism of fibril mineralization, and as a first step we recently determined the size exclusion characteristics of the fibril. This study indicates that apatite crystals up to 12 unit cells in size can access the water within the fibril while molecules larger than a 40-kDa protein are excluded. We proposed a novel mechanism for fibril mineralization based on these observations, one that relies exclusively on agents excluded from the fibril. One agent generates crystals outside the fibril, some of which diffuse into the fibril and grow, and the other selectively inhibits crystal growth outside of the fibril. We have tested this mechanism by examining the impact of removing the major serum inhibitor of apatite growth, fetuin, on the serum-induced calcification of collagen. The results of this test show that fetuin determines the location of serum-driven mineralization: in fetuin's presence, mineral forms only within collagen fibrils; in fetuin's absence, mineral forms only in solution outside the fibrils. The X-ray diffraction spectrum of serum-induced mineral is comparable to the spectrum of bone crystals. These observations show that serum calcification activity consists of an as yet unidentified agent that generates crystal nuclei, some of which diffuse into the fibril, and fetuin, which favors fibril mineralization by selectively inhibiting the growth of crystals outside the fibril.

摘要

骨骼中的矿物质主要位于胶原纤维内,在矿化过程中,纤维先形成,然后纤维内的水被矿物质取代。我们的目标是了解纤维矿化的机制,作为第一步,我们最近确定了纤维的尺寸排阻特性。这项研究表明,尺寸达12个晶胞的磷灰石晶体能够进入纤维内的水,而大于40 kDa的蛋白质分子则被排除在外。基于这些观察结果,我们提出了一种新的纤维矿化机制,该机制完全依赖于被纤维排除的因子。一种因子在纤维外生成晶体,其中一些扩散到纤维内并生长,另一种因子则选择性地抑制纤维外的晶体生长。我们通过研究去除磷灰石生长的主要血清抑制剂胎球蛋白对血清诱导的胶原钙化的影响,来测试这一机制。该测试结果表明,胎球蛋白决定了血清驱动矿化的位置:在有胎球蛋白存在时,矿物质仅在胶原纤维内形成;在无胎球蛋白时,矿物质仅在纤维外的溶液中形成。血清诱导矿物质的X射线衍射光谱与骨晶体的光谱相当。这些观察结果表明,血清钙化活性由一种尚未确定的产生晶核的因子和胎球蛋白组成,其中一些晶核扩散到纤维内,而胎球蛋白通过选择性抑制纤维外晶体的生长来促进纤维矿化。

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