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SIBLING家族成员骨唾液蛋白在骨骼生物学中的作用——小鼠实验遗传学的贡献

The role of the SIBLING, Bone Sialoprotein in skeletal biology - Contribution of mouse experimental genetics.

作者信息

Bouleftour Wafa, Juignet Laura, Bouet Guenaelle, Granito Renata Neves, Vanden-Bossche Arnaud, Laroche Norbert, Aubin Jane E, Lafage-Proust Marie-Hélène, Vico Laurence, Malaval Luc

机构信息

Université de Lyon - Université Jean Monnet, INSERM U1059-LBTO/IFRESIS, Faculté de Médecine, 10 Chemin de la Marandière, St Priest en Jarez F42270, France.

Department of Haematology, University of Cambridge and NHS Blood and Transplant, Cambridge, UK.

出版信息

Matrix Biol. 2016 May-Jul;52-54:60-77. doi: 10.1016/j.matbio.2015.12.011. Epub 2016 Jan 5.

Abstract

Bone Sialoprotein (BSP) is a member of the "Small Integrin-Binding Ligand N-linked Glycoproteins" (SIBLING) extracellular matrix protein family of mineralized tissues. BSP has been less studied than other SIBLING proteins such as Osteopontin (OPN), which is coexpressed with it in several skeletal cell types. Here we review the contribution of genetically engineered mice (BSP gene knockout and overexpression) to the understanding of the role of BSP in the bone organ. The studies made so far highlight the role of BSP in skeletal mineralization, as well as its importance for proper osteoblast and osteoclast differentiation and activity, most prominently in primary/repair bone. The absence of BSP also affects the local environment of the bone tissue, in particular hematopoiesis and vascularization. Interestingly, lack of BSP induces an overexpression of OPN, and the cognate protein could be responsible for some aspects of the BSP gene knockout skeletal phenotype, while replacing BSP for some of its functions. Such interplay between the partly overlapping functions of SIBLING proteins, as well as the network of cross-regulations in which they are involved should now be the focus of further work.

摘要

骨唾液酸蛋白(BSP)是矿化组织中“小整合素结合配体N-连接糖蛋白”(SIBLING)细胞外基质蛋白家族的成员。与其他SIBLING蛋白(如骨桥蛋白,在几种骨骼细胞类型中与BSP共表达)相比,对BSP的研究较少。在此,我们综述了基因工程小鼠(BSP基因敲除和过表达)对理解BSP在骨器官中作用的贡献。迄今为止的研究突出了BSP在骨骼矿化中的作用,以及其对成骨细胞和破骨细胞正常分化及活性的重要性,这在初级/修复骨中最为显著。BSP的缺失也会影响骨组织的局部环境,特别是造血和血管生成。有趣的是,缺乏BSP会诱导骨桥蛋白的过表达,并且同源蛋白可能对BSP基因敲除骨骼表型的某些方面负责,同时替代BSP行使其部分功能。SIBLING蛋白部分重叠功能之间的这种相互作用,以及它们所涉及的交叉调节网络,现在应该成为进一步研究的重点。

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