R J Metz, K Vellody, S Patel, R Bergstrom, J Meisinger, J Jackson, M A Wright, M R Young
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引用次数: 0
摘要
增加蛋白激酶A (PKA)的磷酸化反应或减少蛋白磷酸酶2a (PP-2A)的去磷酸化反应会增加Lewis肺癌(LLC)细胞的侵袭性,这是通过细胞外基质(ECM)包被过滤器的能力来测量的。与非转移性LLC-C8变体相比,转移性LLC-LN7变体降低了PP-2A活性。免疫印迹显示,PP-2A活性水平的降低不是由于PP-2A催化(C)亚基水平的降低。将c2 -神经酰胺添加到lc - ln7裂解物中,或将细胞与c2 -神经酰胺或维生素D3的非钙化类似物孵育,可以刺激细胞的PP-2A活性,后者已被证明可以刺激神经酰胺的释放。这些提高转移性LLC-LN7细胞中PP-2A活性的处理导致其通过选择(ECM)组分,特别是通过玻璃体连接蛋白和层粘连蛋白入侵的能力下降。强调PP-2A在限制肿瘤细胞侵袭性方面的重要性的是,证明过表达PP-2A C α亚基的LLC-LN7细胞转染物通过ECM组分的侵袭性比野生型细胞小。通过与c2 -神经酰胺或维生素D3类似物孵育,进一步增加PP-2A活性,进一步减少这些细胞的侵袭。这些结果表明,维生素D3/神经酰胺/PP-2A途径通过选择ECM成分限制肿瘤细胞的侵袭性。
Vitamin D3 and ceramide reduce the invasion of tumor cells through extracellular matrix components by elevating protein phosphatase-2A.
Increasing phosphorylation reactions by protein kinase A (PKA) or reducing dephosphorylation reactions of protein phosphatase-2A (PP-2A) increases the invasiveness of Lewis lung carcinoma (LLC) cells, as measured by their capacity to traverse extracellular matrix (ECM)-coated filters. Metastatic LLC-LN7 variants have reduced PP-2A activity when compared to nonmetastatic LLC-C8 variants. Immunoblotting showed that this reduced level of PP-2A activity was not due to reduced levels of the PP-2A catalytic (C) subunit. The cellular PP-2A activity could be stimulated by addition of C2-ceramide to LLC-LN7 lysates, or by incubating cells with either C2-ceramide or with a noncalcemic analog of vitamin D3, which has previously been shown to stimulate the release of ceramide. These treatments to elevate PP-2A activity in metastatic LLC-LN7 cells resulted in a decline in their capacity to invade through select (ECM) components, particularly through vitronectin and laminin. Underscoring the importance of PP-2A in limiting the invasiveness of tumor cells was the demonstration that LLC-LN7 cell transfectants overexpressing the PP-2A C alpha subunit were less invasive through ECM components than the wild-type cells. Invasion by these cells was further reduced by additionally increasing PP-2A activity by incubation with C2-ceramide or the vitamin D3 analog. These results suggest a role of a vitamin D3/ceramide/PP-2A pathway in limiting the invasiveness of tumor cells through select ECM components.