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首页> 外文期刊>American Journal of Physiology >Vacuolar H+-ATPase in human breast cancer cells with distinct metastatic potential: distribution and functional activity.
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Vacuolar H+-ATPase in human breast cancer cells with distinct metastatic potential: distribution and functional activity.

机译:人乳腺癌细胞中的液泡H + -ATPase具有独特的转移潜力:分布和功能活性。

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摘要

Tumor cells thrive in a hypoxic microenvironment with an acidic extracellular pH. To survive in this harsh environment, tumor cells must exhibit a dynamic cytosolic pH regulatory system. We hypothesize that vacuolar H(+)-ATPases (V-ATPases) that normally reside in acidic organelles are also located at the cell surface, thus regulating cytosolic pH and exacerbating the migratory ability of metastatic cells. Immunocytochemical data revealed for the first time that V-ATPase is located at the plasma membrane of human breast cancer cells: prominent in the highly metastatic and inconspicuous in the lowly metastatic cells. The V-ATPase activities in isolated plasma membranes were greater in highly than in lowly metastatic cells. The proton fluxes via V-ATPase evaluated by fluorescence spectroscopy in living cells were greater in highly than in lowly metastatic cells. Interestingly, lowly metastatic cells preferentially used the ubiquitous Na(+)/H(+) exchanger and HCO(3)(-)-based H(+)-transporting mechanisms, whereas highly metastatic cells used plasma membrane V-ATPases. The highly metastatic cells were more invasive and migratory than the lowly metastatic cells. V-ATPase inhibitors decreased the invasion and migration in the highly metastatic cells. Altogether, these data indicate that V-ATPases located at the plasma membrane are involved in the acquisition of a more metastatic phenotype.
机译:肿瘤细胞在具有酸性细胞外pH的低氧微环境中壮成长。为了在这种恶劣的环境中生存,肿瘤细胞必须表现出动态的细胞质pH调节系统。我们假设正常情况下位于酸性细胞器中的液泡H(+)-ATPases(V-ATPases)也位于细胞表面,从而调节细胞质的pH值并加剧转移细胞的迁移能力。免疫细胞化学数据首次揭示了V-ATPase位于人乳腺癌细胞的质膜上:在高转移性细胞中突出,而在低转移性细胞中则不明显。高分离的质膜中的V-ATPase活性高于低转移性细胞。在活细胞中,通过荧光光谱法评估的通过V-ATPase的质子通量比在低转移细胞中高。有趣的是,低转移性细胞优先使用无处不在的Na(+)/ H(+)交换子和基于HCO(3)(-)的H(+)转运机制,而高度转移性细胞则使用质膜V-ATPase。高转移性细胞比低转移性细胞更具侵袭性和迁移性。 V-ATPase抑制剂减少了高度转移细胞的侵袭和迁移。总之,这些数据表明位于质膜上的V-ATP酶参与了更具转移性的表型的获得。

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