首页> 美国卫生研究院文献>The EMBO Journal >Mice deficient for the secreted glycoprotein SPARC/osteonectin/BM40 develop normally but show severe age-onset cataract formation and disruption of the lens.
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Mice deficient for the secreted glycoprotein SPARC/osteonectin/BM40 develop normally but show severe age-onset cataract formation and disruption of the lens.

机译:缺乏分泌型糖蛋白SPARC /骨连接蛋白/ BM40的小鼠正常发育但表现出严重的老年性白内障形成和晶状体破坏。

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摘要

SPARC (secreted protein acidic and rich in cysteine, also known as osteonectin/BM40) is a secreted Ca2+-binding glycoprotein that interacts with a range of extracellular matrix molecules, including collagen IV. It is widely expressed during embryogenesis, and in vitro studies have suggested roles in the regulation of cell adhesion and proliferation, and in the modulation of cytokine activity. In order to analyse the function of this protein in vivo, the endogenous Sparc locus was disrupted by homologous recombination in murine embryonic stem cells. SPARC-deficient mice (Sparctm1Cam) appear normal and fertile until around 6 months of age, when they develop severe eye pathology characterized by cataract formation and rupture of the lens capsule. The first sign of lens pathology occurs in the equatorial bow region where vacuoles gradually form within differentiating epithelial cells and fibre cells. The lens capsule, however, shows no qualitative changes in the major basal lamina proteins laminin, collagen IV, perlecan or entactin. These mice are an excellent resource for further studies on how SPARC affects cell behaviour in vivo.
机译:SPARC(酸性分泌蛋白,富含半胱氨酸,也称为骨连接蛋白/ BM40)是一种分泌型Ca2 +结合糖蛋白,可与多种细胞外基质分子(包括IV型胶原)相互作用。它在胚胎发生过程中被广泛表达,并且体外研究表明在调节细胞粘附和增殖以及调节细胞因子活性中起着重要作用。为了在体内分析该蛋白的功能,通过在鼠胚胎干细胞中的同源重组破坏了内源性Sparc基因座。缺乏SPARC的小鼠(Sparctm1Cam)出现正常且可育,直到大约6个月大时才出现严重的眼部疾病,其特征是白内障形成和晶状体囊破裂。晶状体病理学的第一个迹象出现在赤道弓形区域,在分化的上皮细胞和纤维细胞内逐渐形成液泡。然而,该晶状体囊在主要的基底层蛋白层粘连蛋白,胶原蛋白IV,Perlecan或entactin中没有显示出质的变化。这些小鼠是进一步研究SPARC如何影响体内细胞行为的极好资源。

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