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thrombospondins:后生动物细胞外基质的保守介质和调节剂。

Thrombospondins: Conserved mediators and modulators of metazoan extracellular matrix.

机构信息

School of Biochemistry, University of Bristol, Bristol, UK.

出版信息

Int J Exp Pathol. 2024 Oct;105(5):136-169. doi: 10.1111/iep.12517. Epub 2024 Sep 12.

Abstract

This review provides a personal overview of significant scientific developments in the thrombospondin field during the course of my career. Thrombospondins are multidomain, multimeric, calcium-binding extracellular glycoproteins with context-specific roles in tissue organisation. They act at cell surfaces and within ECM to regulate cell phenotype and signalling, differentiation and assembly of collagenous ECM, along with tissue-specific roles in cartilage, angiogenesis and synaptic function. More recently, intracellular, homeostatic roles have also been identified. Resolution of structures for the major domains of mammalian thrombospondins has facilitated major advances in understanding thrombospondin biology from molecule to tissue; for example, in illuminating molecular consequences of disease-causing coding mutations in human pseudoachrondroplasia. Although principally studied in vertebrates, thrombospondins are amongst the most ancient of animal ECM proteins, with many invertebrates encoding a single thrombospondin and the thrombospondin gene family of vertebrates originating through gene duplications. Moreover, thrombospondins form one branch of a thrombospondin superfamily that debuted at the origin of metazoans. The super-family includes additional sub-groups, present only in invertebrates, that differ in N-terminal domain organisation, share the distinctive TSP C-terminal region domain architecture and, to the limited extent studied to date, apparently contribute to tissue development and organisation. Finally, major lines of translational research are discussed, related to fibrosis; TSP1, TSP2 and inhibition of angiogenesis; and the alleviation of chronic cartilage tissue pathologies in pseudoachrondroplasia.

摘要

这篇综述回顾了我职业生涯中在血栓调节蛋白领域的重要科学进展。血栓调节蛋白是一种具有多种结构域和多聚体的、结合钙离子的细胞外糖蛋白,在组织形成中具有特定的作用。它们在细胞表面和细胞外基质(ECM)中发挥作用,调节细胞表型和信号转导、胶原蛋白 ECM 的分化和组装,以及在软骨、血管生成和突触功能中的组织特异性作用。最近,还发现了细胞内的稳态作用。哺乳动物血栓调节蛋白主要结构域的结构解析促进了从分子到组织水平上对血栓调节蛋白生物学的深入理解;例如,阐明了人类假性软骨发育不全中致病编码突变的分子后果。尽管主要在脊椎动物中进行研究,但血栓调节蛋白是动物细胞外基质蛋白中最古老的蛋白之一,许多无脊椎动物编码单个血栓调节蛋白,而脊椎动物的血栓调节蛋白基因家族起源于基因重复。此外,血栓调节蛋白是血栓调节蛋白超家族的一个分支,该超家族出现在后生动物的起源时期。该超家族包括其他亚群,仅存在于无脊椎动物中,它们在 N 端结构域组织上存在差异,共享独特的 TSP C 端区域结构域架构,并且在迄今为止有限的研究范围内,显然有助于组织的发育和形成。最后,讨论了与纤维化相关的主要转化研究领域;TSP1、TSP2 和血管生成抑制;以及假性软骨发育不全中慢性软骨组织病变的缓解。

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