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Connexin 43 expression is associated with increased malignancy in prostate cancer cell lines and functions to promote migration

机译:连接蛋白43的表达与前列腺癌细胞系中恶性肿瘤的增加有关并具有促进迁移的功能

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摘要

Impaired expression of connexins, the gap junction subunits that facilitate direct cell-cell communication, have been implicated in prostate cancer growth. To elucidate the crucial role of connexins in prostate cancer progression, we performed a systematic quantitative RT-PCR screening of connexin expression in four representative prostate cancer cell lines across the spectrum of malignancy. Transcripts of several connexin subunits were detected in all four cell lines, and connexin 43 (Cx43) showed marked elevation at both RNA and protein levels in cells with increased metastatic potential. Analysis of gap-junction-mediated intercellular communication revealed homocellular coupling in PC-3 cells, which had the highest Cx43 expression, with minimal coupling in LNCaP cells where Cx43 expression was very low. Treatment with the gap junction inhibitor carbenoxolone or connexin mimetic peptide ACT-1 did not impair cell growth, suggesting that growth is independent of functional gap junctions. PC-3 cells with Cx43 expression reduced by shRNA showed decreased migration in monolayer wound healing assay, as well as decreased transwell invasion capacities when compared to control cells expressing non-targeting shRNA. These results, together with the correlation between Cx43 expression levels and the metastatic capacity of the cell lines, suggest a role of Cx43 in prostate cancer invasion and metastasis.
机译:连接蛋白(间隙连接亚基,促进直接的细胞间通讯)的表达受损,与前列腺癌的生长有关。为了阐明连接蛋白在前列腺癌进展中的关键作用,我们在恶性谱中对四种代表性前列腺癌细胞系中的连接蛋白表达进行了系统的定量RT-PCR筛选。在所有四个细胞系中均检测到几个连接蛋白亚基的转录物,连接蛋白43(Cx43)在具有转移潜力的细胞中,在RNA和蛋白质水平均显示出明显升高。间隙连接介导的细胞间通讯的分析显示PC-3细胞中的同细胞偶联,其具有最高的Cx43表达,而在Cx43表达非常低的LNCaP细胞中具有最小的偶联。间隙连接抑制剂羧苄酮或连接蛋白模拟肽ACT-1的治疗不会损害细胞生长,表明生长与功能性间隙连接无关。与表达非靶向shRNA的对照细胞相比,具有shRNA降低的Cx43表达的PC-3细胞在单层伤口愈合试验中显示出减少的迁移,以及降低的跨孔侵袭能力。这些结果,以及Cx43表达水平与细胞系转移能力之间的相关性,提示Cx43在前列腺癌的侵袭和转移中的作用。

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