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非红血球血影蛋白αII 敲低后,结直肠癌细胞中促炎细胞因子 IL-8 的表达和分泌增加。

Expression and secretion of the pro‑inflammatory cytokine IL‑8 is increased in colorectal cancer cells following the knockdown of non‑erythroid spectrin αII.

机构信息

Medical Clinic I, Biomedical Research Laboratory, University Clinic Frankfurt, D‑60590 Frankfurt am Main, Germany.

出版信息

Int J Oncol. 2020 Jun;56(6):1551-1564. doi: 10.3892/ijo.2020.5026. Epub 2020 Mar 26.

DOI:10.3892/ijo.2020.5026
PMID:32236629
Abstract

Non‑erythroid spectrin αII (SPTAN1) expression is decreased in ~40% of cases of MLH1‑deficient colorectal cancer (CRC). SPTAN1 knockdown reduces cell viability, cellular mobility and cell‑cell contact formation, indicating that the SPTAN1 plays an important role in tumour growth, attachment and in regulating the tumour microenvironment. Changes in the tumour microenvironment can affect the immune response. Therefore, in the present study, proteome arrays were used to analyse the expression of 119 different chemokines and soluble receptors in CRC cell lines in which mutL homologue 1 (MLH1) or SPTAN1 were knocked down. The levels of interleukin (IL)‑8 were significantly increased in the cells in which SPTAN1 was knocked down, both at the mRNA and protein level. ELISA demonstrated that the cells in which SPTAN1 was knocked down secreted increased quantities of IL‑8, and chemotaxis assays revealed the enhanced trafficking of neutrophils, which was induced by media containing higher levels of IL‑8. The IL‑8 receptors, CRCX1 and CRCX2, were expressed in all the cell lines examined; however, their expression was not directly associated with IL‑8 expression. The results of the present study thus demonstrated that CRC cells in which SPTAN1 was knocked down secreted significantly higher levels of IL‑8, which in‑turn increased the migration of neutrophilic granulocytes. As MLH1‑deficient CRC exhibits an increased infiltration of cytotoxic T‑cells and is associated with a decreased SPTAN1 expression, it can thus be hypothesized that CRC with a low SPTAN1 expression may release increased quantities of IL‑8, resulting in increased immune cell infiltration.

摘要

非红血球血影蛋白 αII(SPTAN1)的表达在约 40%的 MLH1 缺陷结直肠癌(CRC)病例中降低。SPTAN1 敲低降低了细胞活力、细胞迁移和细胞-细胞接触形成,表明 SPTAN1 在肿瘤生长、附着和调节肿瘤微环境中发挥重要作用。肿瘤微环境的变化会影响免疫反应。因此,在本研究中,使用蛋白质组芯片分析了 MLH1 或 SPTAN1 敲低的 CRC 细胞系中 119 种不同趋化因子和可溶性受体的表达。在 SPTAN1 敲低的细胞中,白细胞介素(IL)-8 的水平在 mRNA 和蛋白水平均显著增加。ELISA 表明 SPTAN1 敲低的细胞分泌的 IL-8 量增加,趋化运动分析显示,由含有更高水平 IL-8 的培养基诱导的中性粒细胞的迁移增强。在所有检查的细胞系中均表达 IL-8 受体 CRCX1 和 CRCX2;然而,它们的表达与 IL-8 的表达没有直接关联。因此,本研究的结果表明,SPTAN1 敲低的 CRC 细胞分泌的 IL-8 水平显著升高,进而增加中性粒细胞的迁移。由于 MLH1 缺陷 CRC 表现出细胞毒性 T 细胞浸润增加,并且与 SPTAN1 表达降低相关,因此可以假设 SPTAN1 表达较低的 CRC 可能会释放更多数量的 IL-8,导致免疫细胞浸润增加。

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