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Ion channels in death and differentiation of prostate cancer cells.

机译:前列腺癌细胞死亡和分化中的离子通道。

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Plasma membrane ion channels contribute to virtually all basic cellular processes, including such crucial ones for maintaining tissue homeostasis as proliferation, differentiation, and apoptosis. Enhanced proliferation, aberrant differentiation, and impaired ability to die are the prime reasons for abnormal tissue growth, which can eventually turn into uncontrolled expansion and invasion, characteristic of cancer. Prostate cancer (PCa) cells express a variety of plasma membrane ion channels. By providing the influx of essential signaling ions, perturbing intracellular ion concentrations, regulating cell volume, and maintaining membrane potential, PCa cells are critically involved in proliferation, differentiation, and apoptosis. PCa cells of varying metastatic ability can be distinguished by their ion channel characteristics. Increased malignancy and invasiveness of androgen-independent PCa cells is generally associated with the shift to a 'more excitable' phenotype of their plasma membrane. This shiftis manifested by the appearance of voltage-gated Na(+) and Ca(2+) channels which contribute to their enhanced apoptotic resistance together with downregulated store-operated Ca(2+) influx, altered expression of different K(+) channels and members of the Transient Receptor Potential (TRP) channel family, and strengthened capability for maintaining volume constancy. The present review examines channel types expressed by PCa cells and their involvement in metastatic behaviors.
机译:质膜离子通道实际上参与了所有基本的细胞过程,包括维持组织动态平衡(如增殖,分化和凋亡)的关键过程。增强的增殖,异常分化和受损的死亡能力是异常组织生长的主要原因,其最终可能变成不受控制的扩张和侵袭,这是癌症的特征。前列腺癌(PCa)细胞表达多种质膜离子通道。通过提供基本信号离子的流入,扰动细胞内离子浓度,调节细胞体积并维持膜电位,PCa细胞至关重要地参与了增殖,分化和凋亡。具有不同转移能力的PCa细胞可以通过其离子通道特性来区分。雄激素非依赖性PCa细胞的恶性程度和侵袭性增加通常与其质膜向“更易激发”表型的转变有关。电压门控Na(+)和Ca(2+)通道的出现表明了这种转变,这有助于增加细胞凋亡的抵抗力,以及下调存储操作的Ca(2+)内流,改变了不同K(+)通道的表达和瞬态受体电位(TRP)通道家族的成员,并增强了保持体积恒定的能力。本审查审查了PCa细胞表达的通道类型及其在转移行为中的参与。

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