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IGD 运动潜能的多因素调制在 MSF(迁移刺激因子)中。

Multi-factorial modulation of IGD motogenic potential in MSF (migration stimulating factor).

机构信息

Unit of Cell and Molecular Biology, The Dental School, College of Medicine, Dentistry and Nursing, University of Dundee, Park Place, DD1 4 HR, UK.

出版信息

Exp Cell Res. 2010 Sep 10;316(15):2465-76. doi: 10.1016/j.yexcr.2010.04.003. Epub 2010 Apr 18.

Abstract

Migration Stimulating Factor (MSF) is a genetically truncated isoform of fibronectin (Fn). MSF is a potent stimulator of fibroblast migration, whereas full length Fn is devoid of motogenic activity. MSF and Fn contain four IGD motifs, located in the 3rd, 5th, 7th and 9th type I modules; these modules are referred to as (3)FnI, (5)FnI, (7)FnI and (9)FnI, respectively. We have previously reported that mutation of IGD motifs in modules (7)FnI and (9)FnI of MSF is sufficient to completely abolish the motogenic response of target adult skin fibroblasts. We now report that the IGD sequences in (3)FnI and (5)FnI are also capable of exhibiting motogenic activity when present within fragments of MSF. When present within (1-5)FnI, these sequences require the presence of serum or vitronectin for their motogenic activity to be manifest, whereas the IGD sequences in (7)FnI and (9)FnI are bioactive in the absence of serum factors. All MSF and IGD-containing peptides stimulated the phosphorylation of the integrin binding protein focal adhesion kinase (FAK) but did not necessarily affect migration. These results suggest that steric hindrance determines the motogenic activity of MSF and Fn, and that both molecules contain cryptic bioactive fragments.

摘要

迁移刺激因子(MSF)是纤连蛋白(Fn)的基因截断同工型。MSF 是成纤维细胞迁移的有效刺激物,而全长 Fn 则没有促迁移活性。MSF 和 Fn 含有四个 IGD 基序,位于第 3、5、7 和 9 个 I 型模块中;这些模块分别称为(3)FnI、(5)FnI、(7)FnI 和(9)FnI。我们之前报道过,MSF 中模块(7)FnI 和(9)FnI 的 IGD 基序突变足以完全消除靶成年皮肤成纤维细胞的促迁移反应。我们现在报告说,(3)FnI 和(5)FnI 中的 IGD 序列在 MSF 片段中也能够表现出促迁移活性。当存在于(1-5)FnI 中时,这些序列需要存在血清或 vitronectin 才能表现出其促迁移活性,而(7)FnI 和(9)FnI 中的 IGD 序列在没有血清因子的情况下是生物活性的。所有含有 MSF 和 IGD 的肽都刺激整合素结合蛋白粘着斑激酶(FAK)的磷酸化,但不一定影响迁移。这些结果表明,空间位阻决定了 MSF 和 Fn 的促迁移活性,并且这两种分子都含有隐藏的生物活性片段。

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