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Connecting copper and cancer: from transition metal signalling to metalloplasia

NATURE REVIEWS CANCER (2022)

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Journal

NATURE REVIEWS CANCER
Volume 22, Issue 2, Pages 102-113

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s41568-021-00417-2

Keywords

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Categories

Oncology

Funding

  1. NIH [GM79465, GM139245, GM124749, R01-GM084176, GM120211, GM111672, R21-GM129592, R01-NS109307, CA190265, DK116859, Z01 HD008768, Z01 HD008892, CA53840, DK124907, R01-GM101502, R01-DK117396, R01-DK071865]
  2. US National Cancer Institute [R21CA184788]
  3. Welch Foundation [A-1810]
  4. Pew Charitable Trusts (Pew Scholars Program in Biomedical Science) [50350]
  5. AIRC Italy [IG 17118]
  6. Florida Department of Health Bankhead-Coley Cancer Research Program [9BC07]
  7. Breast Cancer Research Foundation
  8. Susan G. Komen Greater New York City
  9. US Department of Army [W81XH-20-1-0754]
  10. CSHL Cancer Centre Support Grant [CA45508]
  11. V Foundation Scholar Award [3C59 8ABS 3424 3BDA]
  12. Center on the Physics of Cancer Metabolism from the National Cancer Institute [U54CA210184]
  13. National Cancer Institute [R01 CA257254-01A1]
  14. NIDDK [R01-DK-071111]
  15. NIDDK Center grants [P30-DK-41296, P30-DK-020541]
  16. NCI Center grant [P30-CA-13330]
  17. National Health and Medical Research Council of Australia

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Copper is a essential nutrient with both beneficial and toxic properties to cells. Recent progress in transition metal signaling has led to new connections between researchers from different disciplines, with potential for translating basic research into clinical therapies for diseases. The relationship between copper and cancer is particularly important, with opportunities for leveraging disease vulnerabilities through copper-dependent signaling pathways.
Copper is an essential nutrient whose redox properties make it both beneficial and toxic to the cell. Recent progress in studying transition metal signalling has forged new links between researchers of different disciplines that can help translate basic research in the chemistry and biology of copper into clinical therapies and diagnostics to exploit copper-dependent disease vulnerabilities. This concept is particularly relevant in cancer, as tumour growth and metastasis have a heightened requirement for this metal nutrient. Indeed, the traditional view of copper as solely an active site metabolic cofactor has been challenged by emerging evidence that copper is also a dynamic signalling metal and metalloallosteric regulator, such as for copper-dependent phosphodiesterase 3B (PDE3B) in lipolysis, mitogen-activated protein kinase kinase 1 (MEK1) and MEK2 in cell growth and proliferation and the kinases ULK1 and ULK2 in autophagy. In this Perspective, we summarize our current understanding of the connection between copper and cancer and explore how challenges in the field could be addressed by using the framework of cuproplasia, which is defined as regulated copper-dependent cell proliferation and is a representative example of a broad range of metalloplasias. Cuproplasia is linked to a diverse array of cellular processes, including mitochondrial respiration, antioxidant defence, redox signalling, kinase signalling, autophagy and protein quality controlidentifying and characterizing new modes of copper-dependent signalling offers translational opportunities that leverage disease vulnerabilities to this metal nutrient.

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