4.5 Article

Zinc transporters and dysregulated channels in cancers

Journal

FRONTIERS IN BIOSCIENCE-LANDMARK
Volume 22, Issue -, Pages 623-643

Publisher

FRONTIERS IN BIOSCIENCE INC
DOI: 10.2741/4507

Keywords

Zn Homeostasis; ZnT; ZIP; TRP Channels; Store-operated Ca2+ Entry; Orai Channels; STIM; Prostate Cancer; Breast Cancer; Esophageal Cancer; Review

Funding

  1. NIH-NCI [R01-CA185055]
  2. UMDNJ Foundation [62-09]
  3. Pelotonia
  4. Rural and Environment Science and Analytical Services of the Scottish Government
  5. Region Hauts-de-France

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As a nutritionally essential metal ion, zinc (Zn) not only constitutes a structural element for more than 3000 proteins but also plays important regulatory functions in cellular signal transduction. Zn homeostasis is tightly controlled by regulating the flux of Zn across cell membranes through specific transporters, i.e. ZnT and ZIP family proteins. Zn deficiency and malfunction of Zn transporters have been associated with many chronic diseases including cancer. However, the mechanisms underlying Zn regulatory functions in cellular signaling and their impact on the pathogenesis and progression of cancers remain largely unknown. In addition to these acknowledged multifunctions, Zn modulates a wide range of ion channels that in turn may also play an important role in cancer biology. The goal of this review is to propose how zinc deficiency, through modified Zn homeostasis, transporter activity and the putative regulatory function of Zn can influence ion channel activity, and thereby contribute to carcinogenesis and tumorigenesis. This review intends to stimulate interest in, and support for research into the understanding of Zn-modulated channels in cancers, and to search for novel biomarkers facilitating effective clinical stratification of high risk cancer patients as well as improved prevention and therapy in this emerging field.

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