细胞迁移
运动性
生物
肌动蛋白
异位表达
转移
癌症研究
腺癌
细胞生物学
细胞
淋巴结
肿瘤进展
病理
原发性肿瘤
细胞培养
肺腺癌
肺
细胞生长
基因表达
内生
CD44细胞
肿瘤微环境
人口
癌症
作者
Sabine Windhorst,Т. С. Калинина,Katharina Schmid,Christine Blechner,Neele Kriebitzsch,Robin Hinsch,Lydia Chang,Lena Herich,Udo Schumacher,Georg W. Mayr
摘要
Abstract Cell migration is one of the hallmarks of metastatic disease and thus identification of migration promoting proteins is crucial for the understanding of metastasis formation. Here we show that the neuron‐specific, F‐actin bundling inositol‐1,4,5‐trisphosphate‐3‐kinase‐A (ITPKA) is ectopically expressed in tumor cells and critically involved in migration. Down‐regulation of ITPKA expression in transformed cell‐lines with ectopic expression of ITPKA significantly decreased migration and the number of linear and branched cell protrusion. Conversely, up‐regulation of ITPKA in tumor cell lines with low endogenous ITPKA expression increased migration and formation of cell processes. In vitro , ITPKA alone induced the formation of linear actin filaments, whereas ITPKA mediated formation of branched protrusions seems to result from interaction between ITPKA and the F‐actin cross‐linking protein filamin C. Based on these actin‐modulating and migration‐promoting effects of ITPKA we examined its expression in clinical samples of different tumor entities, starting with the analysis of multiple tumor tissue arrays. As in lung adenocarcinoma specimens, the highest ITPKA expression rate was found, this tumor entity was examined in more detail. ITPKA was expressed early in adenocarcinoma progression (pN0) and was largely maintained in invasive and metastatic tumor cell populations (pN1/2, lymph node metastases). Together with our result that high expression of ITPKA increases motility of tumor cells we conclude that the observed expression of ITPKA early in tumor development increases the metastatic potential of lung adenocarcinoma cells. Therefore, we suggest that ITPKA may be a promising therapeutic molecular target for anti metastatic therapy of lung cancer.
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