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鉴定一种弹性蛋白衍生的趋化肽VGVAPG的肿瘤细胞受体。

Identification of a tumor cell receptor for VGVAPG, an elastin-derived chemotactic peptide.

作者信息

Blood C H, Sasse J, Brodt P, Zetter B R

机构信息

Department of Cellular Physiology, Children's Hospital, Boston, MA 02115.

出版信息

J Cell Biol. 1988 Nov;107(5):1987-93. doi: 10.1083/jcb.107.5.1987.

Abstract

Extracellular matrix proteins and their proteolytic products have been shown to modulate cell motility. We have found that certain tumor cells display a chemotactic response to degradation products of the matrix protein elastin, and to an elastin-derived peptide, VGVAPG. The hexapeptide VGVAPG is a particularly potent chemotaxin for lung-colonizing Lewis lung carcinoma cells (line M27), with 5 nM VGVAPG eliciting maximal chemotactic response when assayed in 48-microwell chemotaxis chambers. Binding of the elastin-derived peptide to M27 cells was studied using a tyrosinated analog (Y-VGVAPG) to allow iodination. Scatchard analysis of [125I]Y-VGVAPG binding to viable M27 tumor cells at both 37 and 4 degrees C indicates the presence of a single class of high affinity binding sites. The dissociation constant obtained from these studies (2.7 X 10(-9) M) is equivalent to the concentration of VGVAPG required for chemotactic activity. The receptor molecule was identified as an Mr 59,000 species by covalent cross-linking of the radiolabeled ligand to the M27 tumor cell surface and subsequent analysis of the cross-linked material by electrophoresis and size-exclusion high performance liquid chromatography. These results suggest that M27 tumor cell chemotaxis to VGVAPG is initiated by high affinity binding of the peptide to a distinct cell surface receptor.

摘要

细胞外基质蛋白及其蛋白水解产物已被证明可调节细胞运动。我们发现某些肿瘤细胞对基质蛋白弹性蛋白的降解产物以及一种弹性蛋白衍生肽VGVAPG表现出趋化反应。六肽VGVAPG对定殖于肺部的Lewis肺癌细胞(M27系)是一种特别有效的趋化因子,在48孔趋化室中进行测定时,5 nM的VGVAPG可引发最大趋化反应。使用酪氨酸化类似物(Y-VGVAPG)进行碘化,研究了弹性蛋白衍生肽与M27细胞的结合。在37℃和4℃下对[125I]Y-VGVAPG与存活的M27肿瘤细胞的结合进行Scatchard分析,结果表明存在一类单一的高亲和力结合位点。从这些研究中获得的解离常数(2.7×10^(-9) M)与趋化活性所需的VGVAPG浓度相当。通过将放射性标记的配体与M27肿瘤细胞表面进行共价交联,并随后通过电泳和尺寸排阻高效液相色谱法对交联物质进行分析,将受体分子鉴定为一种分子量为59,000的物质。这些结果表明,M27肿瘤细胞对VGVAPG的趋化作用是由该肽与一种独特的细胞表面受体的高亲和力结合引发的。

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