粒细胞集落刺激因子受体促进β1整合素介导的膀胱癌细胞黏附和侵袭。

Granulocyte colony-stimulating receptor promotes beta1-integrin-mediated adhesion and invasion of bladder cancer cells.

作者信息

Chakraborty Arup, White Scott M, Guha Sushovan

机构信息

Section of Leukocyte Biology, Department of Pediatrics, Baylor College of Medicine, Houston, Texas 77030, USA.

出版信息

Urology. 2006 Jul;68(1):208-13. doi: 10.1016/j.urology.2006.01.046.

DOI:10.1016/j.urology.2006.01.046

PMID:16844458

Abstract

OBJECTIVES

To determine whether granulocyte colony-stimulating factor receptor (G-CSFR) autocrine signaling promotes endothelial cell adhesion and invasion of bladder cancer cells through a beta1-integrin-mediated pathway. A significant fraction of invasive bladder carcinomas express both G-CSF and G-CSFR. Bladder carcinoma cell line 5637 constitutively secretes G-CSF but lacks G-CSFR expression. Thus, we studied the effects of G-CSFR expression on cell adhesion and invasion in this unique model system.

METHODS

Flow cytometry and adhesion assay were performed to detect expression of beta1-integrin in G-CSFR-expressing 5637 cells and adhesion of these cells to human umbilical vein endothelial cell, respectively. Furthermore, an invasion chamber assay was done with the 5637 cells. Next, we used the G-CSF-specific antibody, siRNA, and a truncated version of G-CSFR (GR19) to block G-CSFR autocrine loop in these cells. We also used a beta1-integrin-specific neutralizing antibody in the adhesion and invasion assays with the 5637 cells.

RESULTS

G-CSFR-mediated increased expression (approximately threefold) of beta1-integrin is significantly abrogated by G-CSF specific antibody or siRNA in 5637 cells. GR19 also completely blocked beta1-integrin expression. G-CSFR signaling increased adhesion (approximately 2.5-fold) of 5637 cells to human umbilical vein endothelial cells, which are potently blocked by beta1-integrin-specific antibody. G-CSF/G-CSFR autocrine signaling significantly increased the invasiveness of 5637 cells (approximately 10-fold), which was reduced by either attenuating G-CSF production (G-CSF-specific antibody and siRNA) or interfering with G-CSFR signaling (GR19). Furthermore, beta1-integrin-specific antibody completely blocked G-CSFR-mediated invasion of 5637 cells.

CONCLUSIONS

Autocrine G-CSF/G-CSFR signaling in bladder cancer can significantly contribute to cancer cell adhesion and invasion in a beta1-integrin-dependent manner.

摘要

目的

确定粒细胞集落刺激因子受体（G-CSFR）自分泌信号是否通过β1整合素介导的途径促进膀胱癌细胞的内皮细胞黏附和侵袭。相当一部分浸润性膀胱癌同时表达G-CSF和G-CSFR。膀胱癌细胞系5637组成性分泌G-CSF，但缺乏G-CSFR表达。因此，我们在这个独特的模型系统中研究了G-CSFR表达对细胞黏附和侵袭的影响。

方法

分别进行流式细胞术和黏附试验，以检测表达G-CSFR的5637细胞中β1整合素的表达以及这些细胞与人脐静脉内皮细胞的黏附。此外，对5637细胞进行侵袭小室试验。接下来，我们使用G-CSF特异性抗体、小干扰RNA（siRNA）和G-CSFR的截短版本（GR19）来阻断这些细胞中的G-CSFR自分泌环。我们还在对5637细胞的黏附和侵袭试验中使用了β1整合素特异性中和抗体。

结果

在5637细胞中，G-CSF特异性抗体或siRNA可显著消除G-CSFR介导的β1整合素表达增加（约三倍）。GR19也完全阻断了β1整合素的表达。G-CSFR信号增强了5637细胞与人脐静脉内皮细胞的黏附（约2.5倍），而β1整合素特异性抗体可有效阻断这种黏附。G-CSF/G-CSFR自分泌信号显著增加了5637细胞的侵袭性（约10倍），通过减少G-CSF产生（G-CSF特异性抗体和siRNA）或干扰G-CSFR信号（GR19）可降低这种侵袭性。此外，β1整合素特异性抗体完全阻断了G-CSFR介导的5637细胞侵袭。