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二聚化和底物排斥在骨形态发生蛋白-1和哺乳动物类 tolloid 调控中的作用

Role of dimerization and substrate exclusion in the regulation of bone morphogenetic protein-1 and mammalian tolloid.

作者信息

Berry Richard, Jowitt Thomas A, Ferrand Johanna, Roessle Manfred, Grossmann J Günter, Canty-Laird Elizabeth G, Kammerer Richard A, Kadler Karl E, Baldock Clair

机构信息

Wellcome Trust Centre for Cell-Matrix Research, Faculty of Life Sciences, University of Manchester, Manchester M13 9PT, United Kingdom.

出版信息

Proc Natl Acad Sci U S A. 2009 May 26;106(21):8561-6. doi: 10.1073/pnas.0812178106. Epub 2009 May 8.

DOI:10.1073/pnas.0812178106
PMID:19429706
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2689009/
Abstract

The bone morphogenetic protein (BMP)-1/tolloid metalloproteinases are evolutionarily conserved enzymes that are fundamental to dorsal-ventral patterning and tissue morphogenesis. The lack of knowledge regarding how these proteinases recognize and cleave their substrates represents a major hurdle to understanding tissue assembly and embryonic patterning. Although BMP-1 and mammalian tolloid (mTLD) are splice variants, it is puzzling why BMP-1, which lacks 3 of the 7 noncatalytic domains present in all other family members, is the most effective proteinase. Using a combination of single-particle electron microscopy, small-angle X-ray scattering, and other biophysical measurements in solution, we show that mTLD, but not BMP-1, forms a calcium-ion-dependent dimer under physiological conditions. Using a domain deletion approach, we provide evidence that EGF2, which is absent in BMP-1, is critical to the formation of the dimer. Based on a combination of structural and functional data, we propose that mTLD activity is regulated by a substrate exclusion mechanism. These results provide a mechanistic insight into how alternative splicing of the Bmp1 gene produces 2 proteinases with differing biological activities and have broad implications for regulation of BMP-1/mTLD and related proteinases during BMP signaling and tissue assembly.

摘要

骨形态发生蛋白(BMP)-1/类 tolloid 金属蛋白酶是进化上保守的酶,对背腹模式形成和组织形态发生至关重要。对于这些蛋白酶如何识别和切割其底物的了解不足,是理解组织组装和胚胎模式形成的主要障碍。尽管 BMP-1 和哺乳动物类 tolloid(mTLD)是剪接变体,但令人费解的是,BMP-1 在所有其他家族成员中存在的 7 个非催化结构域中缺少 3 个,却是最有效的蛋白酶。通过结合单颗粒电子显微镜、小角 X 射线散射和溶液中的其他生物物理测量,我们表明,在生理条件下,mTLD 而非 BMP-1 形成钙离子依赖性二聚体。使用结构域缺失方法,我们提供证据表明 BMP-1 中不存在的 EGF2 对二聚体的形成至关重要。基于结构和功能数据的结合,我们提出 mTLD 活性受底物排斥机制调节。这些结果为 Bmp1 基因的可变剪接如何产生具有不同生物学活性的两种蛋白酶提供了机制性见解,并对 BMP 信号传导和组织组装过程中 BMP-1/mTLD 及相关蛋白酶的调节具有广泛影响。

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The interaction of recombinant subdomains of the procollagen C-proteinase with procollagen I provides a quantitative explanation for functional differences between the two splice variants, mammalian tolloid and bone morphogenetic protein 1.前胶原C蛋白酶的重组亚结构域与I型前胶原的相互作用为两种剪接变体(哺乳动物类 tolloid 和骨形态发生蛋白1)之间的功能差异提供了定量解释。
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