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首页> 美国卫生研究院文献>NPG Open Access >The interactome of metabolic enzyme carbonic anhydrase IX reveals novel roles in tumor cell migration and invadopodia/MMP14-mediated invasion
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The interactome of metabolic enzyme carbonic anhydrase IX reveals novel roles in tumor cell migration and invadopodia/MMP14-mediated invasion

机译:代谢酶碳酸酐酶IX的相互作用组揭示了肿瘤细胞迁移和invadopodia / MMP14介导的侵袭中的新作用

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Carbonic anhydrase IX (CAIX) is a hypoxia inducible factor 1-induced, cell surface pH regulating enzyme with an established role in tumor progression and clinical outcome. However, the molecular basis of CAIX-mediated tumor progression remains unclear. Here, we have utilized proximity dependent biotinylation (BioID) to map the CAIX ‘interactome’ in breast cancer cells in order to identify physiologically relevant CAIX-associating proteins with potential roles in tumor progression. High confidence proteins identified include metabolic transporters, β1 integrins, integrin-associated protein CD98hc and matrix metalloprotease 14 (MMP14). Biochemical studies validate the association of CAIX with α2β1 integrin, CD98hc and MMP14, and immunofluorescence microscopy demonstrates colocalization of CAIX with α2β1 integrin and MMP14 in F-actin/cofilin-positive lamellipodia/pseudopodia, and with MMP14 to cortactin/Tks5-positive invadopodia. Modulation of CAIX expression and activity results in significant changes in cell migration, collagen degradation and invasion. Mechanistically, we demonstrate that CAIX associates with MMP14 through potential phosphorylation residues within its intracellular domain, and that CAIX enhances MMP14-mediated collagen degradation by directly contributing hydrogen ions required for MMP14 catalytic activity. These findings establish hypoxia-induced CAIX as a novel metabolic component of cellular migration and invasion structures, and provide new mechanistic insights into its role in tumor cell biology.
机译:碳酸酐酶IX(CAIX)是一种缺氧诱导因子1诱导的细胞表面pH调节酶,在肿瘤的进展和临床结果中具有确定的作用。但是,CAIX介导的肿瘤进展的分子基础仍然不清楚。在这里,我们利用邻近依赖性生物素化(BioID)来绘制乳腺癌细胞中的CAIX“相互作用组”图谱,以鉴定在肿瘤进展中具有潜在作用的生理相关的CAIX相关蛋白。鉴定出的高可信度蛋白质包括代谢转运蛋白,β1整合素,整合素相关蛋白质CD98hc和基质金属蛋白酶14(MMP14)。生化研究证实了CAIX与α2β1整合素,CD98hc和MMP14的关联,并且免疫荧光显微镜检查证明CAIX与α2β1整合素和MMP14在F-肌动蛋白/ cofilin阳性的lamellipodia /假性伪足中共定位,并与MMP14结合到cortactin / Tks5的阳性In。 CAIX表达和活性的调节导致细胞迁移,胶原蛋白降解和侵袭的显着变化。从机理上讲,我们证明CAIX通过其细胞内结构域中的潜在磷酸化残基与MMP14缔合,并且CAIX通过直接贡献MMP14催化活性所需的氢离子来增强MMP14介导的胶原蛋白降解。这些发现将缺氧诱导的CAIX确立为细胞迁移和侵袭结构的新陈代谢成分,并为其在肿瘤细胞生物学中的作用提供了新的机理见解。

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