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首页> 外文期刊>Journal of Cancer Research and Clinical Oncology >Locomotion of tumor cells: a molecular comparison to migrating pre- and postmitotic leukocytes.
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Locomotion of tumor cells: a molecular comparison to migrating pre- and postmitotic leukocytes.

机译:肿瘤细胞的运动:与有丝分裂前和有丝分裂后白细胞迁移的分子比较。

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Increasing evidence has shown that the molecular regulation of active cell migration of slow-moving cells, e.g., tumor cells and fibroblasts, is different from fast-moving leukocytes, e.g., T lymphocytes and neutrophil granulocytes. Slow-moving cells develop focal adhesions as a crucial regulatory element during migration. These focal adhesions connect the extracellular matrix to the intracellular actin- and tubulin-cytoskeleton via integrins and enzymatically active proteins. Beside matrix-binding integrins, ligands of receptor tyrosine kinases and heterotrimeric G protein-coupled serpentine receptors initiate migration of slow-moving cells. Focal adhesions are not found in T lymphocytes and neutrophil granulocytes moving within three-dimensional matrices. In T lymphocytes, the T cell receptor is supposed to have a key regulatory function not only in antigen recognition, cell activation, and proliferation but also in cell migration. Regulatory molecules as well as the cytoskeleton are connected to the T cell receptor. The T cell receptor functionally combines elements of receptor tyrosine kinase signaling and of focal adhesions. In neutrophil granulocytes no multi-protein complexes regulating migration have been identified so far. Most potent activators of migration of neutrophil granulocytes, as those of T lymphocytes, are chemokines binding to heterotrimeric G protein-coupled serpentine receptors.
机译:越来越多的证据表明,缓慢移动的细胞(例如肿瘤细胞和成纤维细胞)的活性细胞迁移的分子调控不同于快速移动的白细胞(例如T淋巴细胞和嗜中性粒细胞)。缓慢移动的细胞在迁移过程中将黏着斑作为重要的调节元件。这些粘着粘附通过整联蛋白和酶活性蛋白将细胞外基质连接至细胞内肌动蛋白和微管蛋白-细胞骨架。除基质结合整联蛋白外,受体酪氨酸激酶的配体和异三聚体G蛋白偶联的蛇纹石受体还启动了缓慢移动的细胞的迁移。在三维矩阵内移动的T淋巴细胞和嗜中性粒细胞中未发现局灶性粘连。在T淋巴细胞中,T细胞受体不仅在抗原识别,细胞活化和增殖方面而且在细胞迁移方面都具有关键的调节功能。调节分子以及细胞骨架都与T细胞受体相连。 T细胞受体在功能上结合了受体酪氨酸激酶信号传导和粘着斑的元素。迄今为止,在嗜中性粒细胞中尚未发现调节迁移的多蛋白复合物。与T淋巴细胞一样,嗜中性粒细胞迁移的最有效激活剂是与异三聚体G蛋白偶联的蛇形受体结合的趋化因子。

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