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从胶原蛋白化学到细胞治疗——一段个人历程。

From collagen chemistry towards cell therapy - a personal journey.

作者信息

Grant Michael E

机构信息

Wellcome Trust Centre for Cell-Matrix Research, Faculty of Life Sciences, The University of Manchester, Manchester, UK.

出版信息

Int J Exp Pathol. 2007 Aug;88(4):203-14. doi: 10.1111/j.1365-2613.2007.00537.x.

Abstract

The Fell-Muir Award requires the recipient to deliver a lecture and a review manuscript which provides a personal overview of significant scientific developments in the field of matrix biology over the period of the recipient's career. In this context, this review considers the collagen family of structural proteins and the advances in biochemical, molecular biological and genetic techniques which led to the elucidation of the structure, synthesis and function of this important group of extracellular matrix constituents. Particular attention is focussed on early research on the identification and assembly of the soluble precursors of collagen types I and II, and the identification of the precursor of basement membrane collagen type IV. In subsequent studies investigating the maintenance of the chick chondrocyte phenotype in culture, the influence of the extracellular milieu was found to influence markedly both cell morphology and collagen gene expression. These studies led to the discovery of collagen type X whose expression is restricted to hypertrophic chondrocytes at sites of endochondral ossification. Such research provided a prelude to investigations of mammalian endochondral ossification which is known to be aberrant in a variety of human chondrodysplasias and is reactivated in bone fracture repair and in osteoarthritis. The cloning of bovine and then human collagen type X genes facilitated studies in relevant human diseases and contributed to the discovery of mutations in the COL10A1 gene in families with metaphyseal chondrodysplasia type Schmid. Clustering of mutations in the C-terminal domain of the type X collagen molecule has now been widely documented and investigations of the pathogenic mechanisms in animal models are beginning to suggest the prospect of novel treatment strategies.

摘要

费尔-米尔奖要求获奖者发表一次演讲并撰写一篇综述稿件,该综述稿件需对获奖者职业生涯期间基质生物学领域的重大科学进展进行个人概述。在此背景下,本综述探讨了结构蛋白的胶原蛋白家族,以及生物化学、分子生物学和遗传学技术的进展,这些进展促成了对这一重要细胞外基质成分组的结构、合成和功能的阐明。特别关注的是关于I型和II型胶原蛋白可溶性前体的鉴定和组装的早期研究,以及IV型基底膜胶原蛋白前体的鉴定。在随后研究培养的鸡软骨细胞表型维持的实验中,发现细胞外环境对细胞形态和胶原蛋白基因表达均有显著影响。这些研究促成了X型胶原蛋白的发现,其表达仅限于软骨内骨化部位的肥大软骨细胞。此类研究为哺乳动物软骨内骨化的研究奠定了基础,已知在多种人类软骨发育不良中软骨内骨化异常,且在骨折修复和骨关节炎中会重新激活。牛X型胶原蛋白基因以及随后人类X型胶原蛋白基因的克隆促进了对相关人类疾病的研究,并有助于发现施密德型干骺端软骨发育不良家族中COL10A1基因的突变。现已广泛记录到X型胶原蛋白分子C端结构域的突变聚集情况,对动物模型致病机制的研究开始暗示新治疗策略的前景。

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