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The emerging role of zinc transporters in cellular homeostasis and cancer

机译:锌转运蛋白在细胞稳态和癌症中的新兴作用

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摘要

Zinc is an essential micronutrient that plays a role in the structural or enzymatic functions of many cellular proteins. Cellular zinc homeostasis involves the opposing action of two families of metal transporters: the ZnT (SLC30) family that functions to reduce cytoplasmic zinc concentrations and the ZIP (SLC39) family that functions to increase cytoplasmic zinc concentrations. Fluctuations in intracellular zinc levels mediated by these transporter families affect signaling pathways involved in normal cell development, growth, differentiation and death. Consequently, changes in zinc transporter localization and function resulting in zinc dyshomeostasis have pathophysiological effects. Zinc dyshomeostasis has been implicated in the progression of cancer. Here we review recent progress toward understanding the structural basis for zinc transport by ZnT and ZIP family proteins, as well as highlight the roles of zinc as a signaling molecule in physiological conditions and in various cancers. As zinc is emerging as an important signaling molecule in the development and progression of cancer, the ZnT and ZIP transporters that regulate cellular zinc homeostasis are promising candidates for targeted cancer therapy.
机译:锌是一种必需的微量营养素,在许多细胞蛋白的结构或酶促功能中起作用。细胞锌稳态涉及两个金属转运蛋白家族的相反作用:起到降低细胞质锌浓度的作用的ZnT(SLC30)家族和起增加细胞质锌浓度的功能的ZIP(SLC39)家族。这些转运蛋白家族介导的细胞内锌水平的波动会影响正常细胞发育,生长,分化和死亡所涉及的信号通路。因此,锌转运蛋白定位和功能的改变导致锌异位稳态具有病理生理作用。锌异位稳态与癌症的发展有关。在这里,我们回顾了了解锌通过ZnT和ZIP家族蛋白转运的结构基础的最新进展,并重点介绍了锌作为信号分子在生理状况和各种癌症中的作用。由于锌正在成为癌症发展和进程中的重要信号分子,因此调节细胞锌稳态的ZnT和ZIP转运蛋白有望成为靶向癌症治疗的候选药物。

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