Journal article

The oncogenic roles of TRPM ion channels in cancer

Abstract:: Transient receptor potential (TRP) proteins are a diverse family of ion channels present in multiple types of tissues. They function as gatekeepers for responses to sensory stimuli including temperature, vision, taste, and pain through their activities in conducting ion fluxes. The TRPM (melastatin) subfamily consists of eight members (i.e., TRPM1–8), which collectively regulate fluxes of various types of cations such as K+, Na+, Ca2+, and Mg2+. Growing evidence in the past two decades indicates that TRPM ion channels, their isoforms, or long noncoding RNAs encoded within the locus may be oncogenes involved in the regulation of cancer cell growth, proliferation, autophagy, invasion, and epithelial–mesenchymal transition, and their significant association with poor clinical outcomes of cancer patients. In this review, we describe and discuss recent findings implicating TRPM channels in different malignancies, their functions, mechanisms, and signaling pathways involved in cancers, as well as summarizing their normal physiological functions and the availability of ion channel pharmacological inhibitors.

Publication status:: Published

Peer review status:: Peer reviewed

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APA Style

Wong, K. K., Banham, A., Yaacob, N., & Husna, S. M. N. (2019). The oncogenic roles of TRPM ion channels in cancer. Journal of Cellular Physiology, 234(9), 14556–14573.

MLA Style

Wong, K. K., et al. “The Oncogenic Roles of TRPM Ion Channels in Cancer.” Journal of Cellular Physiology, vol. 234, no. 9, Wiley, 2019, pp. 14556–73.

Chicago Style

Wong, KK, A Banham, N Yaacob, and SMN Husna. 2019. “The Oncogenic Roles of TRPM Ion Channels in Cancer.” Journal of Cellular Physiology 234 (9): 14556–73.
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Files:: The Oncogenic Roles of TRPM Ion Channels in Cancer.pdf

(Preview, Accepted manuscript, pdf, 330.3KB, Terms of use)

Publisher copy:: 10.1002/jcp.28168

Authors

+ Wong, KK More by this author

Role:: Author

+ Banham, A More by this author

Institution:: University of Oxford
Division:: MSD
Department:: RDM
Sub department:: RDM Clinical Laboratory Sciences
Role:: Author
ORCID:: 0000-0002-3197-273X

+ Yaacob, N More by this author

Role:: Author

+ Husna, SMN More by this author

Role:: Author

Publisher:: Wiley
Journal:: Journal of Cellular Physiology More from this journal
Volume:: 234
Issue:: 9
Pages:: 14556-14573
Publication date:: 2019-02-02
Acceptance date:: 2018-11-08
DOI:: 10.1002/jcp.28168
EISSN:: 1097-4652
ISSN:: 0021-9541

Keywords:: TRPM

isoforms

lncRNA

oncogenes
Pubs id:: pubs:965439
UUID:: uuid:fabb30b0-db58-46b5-b4d6-8c7b82a36147
Local pid:: pubs:965439
Source identifiers:: 965439
Deposit date:: 2019-01-21

Terms of use

Copyright holder:: Wiley Periodicals, Inc
Copyright date:: 2019
Rights statement:: © 2019 Wiley Periodicals, Inc.
Notes:: This is the accepted manuscript version of the article. The final version is available online from Wiley at: https://doi.org/10.1002/jcp.28168

Licence:: Terms and Conditions of Use for Oxford University Research Archive

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