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Ovarian cancer: Ion channel and aquaporin expression as novel targets of clinical potential

机译:卵巢癌:离子通道和水通道蛋白表达作为临床潜力的新目标

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摘要

Ovarian cancer is associated with limited overall survival, due to problems in early detection and therapy. Membrane ion channels have been proposed to play a significant, concerted role in the cancer process, from initial proliferation to metastasis, and promise to be early, functional biomarkers. We review the evidence for ion channel and aquaporin expression and functioning in human ovarian cancer cells and tissues. In vitro, K+ channels, mainly voltage-gated, including Ca2+-activated channels, have been found to control the cell cycle, as in other cancers. Voltage-gated, volume-regulated and intracellular Cl- channels have been detected in vitro and in vivo and shown to be involved in proliferation, adhesion and invasion. Evidence for 'transient receptor potential', voltage-gated sodium and calcium channels, which have been shown to contribute to pathogenesis of other carcinomas, is also emerging in ovarian cancer. Aquaporins may be involved in cell growth, migration and formation of ascites via increased water permeability of micro-vessels. It is concluded that functional expression of ion channels and their regulation by steroid hormones and growth factors are an integral part of ovarian cancer development and progression. Furthermore, ion channels may be involved in multidrug resistance, commonly associated with treatment of ovarian cancer. We propose that ion channel studies can facilitate our understanding of the pathobiology of ovarian cancer and, ultimately, can serve as viable novel targets for its clinical management.
机译:由于早期检测和治疗中的问题,卵巢癌与有限的总体生存有关。已经提出,膜离子通道在癌症过程中(从最初的增殖到转移)起着重要的协同作用,并有望成为早期的功能性生物标志物。我们审查了在人类卵巢癌细胞和组织中离子通道和水通道蛋白表达和功能的证据。在体外,与其他癌症一样,已发现主要通过电压门控的K +通道(包括Ca2 +激活的通道)可控制细胞周期。已在体外和体内检测到电压门控,体积调节和细胞内Cl-通道,显示它们参与了增殖,粘附和侵袭。卵巢癌中也出现了“瞬时受体电位”,电压门控钠和钙通道的证据,这些信号已被证明有助于其他癌症的发病。水通道蛋白可能通过增加微血管的透水性而参与细胞的生长,迁移和腹水的形成。结论是,离子通道的功能性表达及其通过类固醇激素和生长因子的调控是卵巢癌发生和发展的组成部分。此外,离子通道可能参与多药耐药性,通常与卵巢癌的治疗有关。我们建议离子通道研究可以促进我们对卵巢癌病理生物学的理解,并最终可以作为其临床治疗的可行新靶标。

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