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血小板反应蛋白-1的淀粉样蛋白样C末端结构域表现出需要两个VVM基序的CD47激动剂活性。

An amyloid-like C-terminal domain of thrombospondin-1 displays CD47 agonist activity requiring both VVM motifs.

作者信息

McDonald J F, Dimitry J M, Frazier W A

机构信息

Department of Biochemistry and Molecular Biophysics, Washington University School of Medicine, Box 8231, 660 South Euclid Avenue, St. Louis, Missouri 63110, USA.

出版信息

Biochemistry. 2003 Aug 26;42(33):10001-11. doi: 10.1021/bi0341408.

Abstract

Two VVM-containing peptides in the C-terminal domain (CBD) of thrombospondin-1 function as CD47 agonists. A recombinant form of the CBD (rCBD) has been expressed that contains both VVM sites and exhibits CD47-dependent binding of C32 melanoma cells when coated at concentrations 100x lower than the peptide 4N1K (kRFYVVMWKk). Circular dichroism and thioflavin T binding of a recombinant form of the C-terminal domain (rCBD) of thrombospondin-1 indicated a species highly enriched in beta-sheet secondary structure, with spectra similar to those of amyloid proteins. Reduction of the CD signal with progressively higher concentrations of guanidine hydrochloride was correlated with a loss of cell-binding activity. Melanoma cell spreading on vitronectin was strongly stimulated by immobilized rCBD co-coated at concentrations more than 50x lower than 4N1K, and the effect was blocked by treatment with pertussis toxin, consistent with the known mediation of CD47 signaling by trimeric G(i). Mutations of either or both VV sequences of rCBD (1037-38 and 1123-24 of TSP1) to GG had a modest effect on cell binding, a component of which was inhibited by heparin. However, all three mutants dramatically reduced the signaling-dependent stimulation of cell spreading, indicating that the VVM motifs of rCBD are structurally linked in CD47 activation.

摘要

血小板反应蛋白-1 C末端结构域(CBD)中的两种含VVM的肽作为CD47激动剂发挥作用。已表达了一种重组形式的CBD(rCBD),其包含两个VVM位点,并且当以比肽4N1K(kRFYVVMWKk)低100倍的浓度包被时,表现出对C32黑色素瘤细胞的CD47依赖性结合。血小板反应蛋白-1 C末端结构域(rCBD)的重组形式的圆二色性和硫黄素T结合表明,该物种富含β-折叠二级结构,其光谱与淀粉样蛋白相似。随着盐酸胍浓度的逐渐升高,CD信号的降低与细胞结合活性的丧失相关。固定化的rCBD以比4N1K低50倍以上的浓度共包被时,强烈刺激黑色素瘤细胞在玻连蛋白上的铺展,并且该效应被百日咳毒素处理所阻断,这与三聚体G(i)介导的CD47信号传导一致。rCBD(TSP1的1037-38和1123-24)的一个或两个VV序列突变为GG对细胞结合有适度影响,其中一部分被肝素抑制。然而,所有三个突变体都显著降低了信号依赖性的细胞铺展刺激,表明rCBD的VVM基序在CD47激活中在结构上是相连的。

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