Molecular Functions and Significance of the MTA Family in Hormone-Independent Cancer
Document Type
Article
Publication Date
2014
Abstract
The members of the metastasis-associated protein (MTA) family play pivotal roles in both physiological and pathophysiological processes, especially in cancer development and metastasis, and their role as master regulators has come to light. Due to the fact that they were first identified as crucial factors in estrogen receptor-mediated breast cancer metastasis, most of the early studies focused on their hormone-dependent functions. However, the accumulating evidence shows that the members of MTA family are deregulated in most, if not all, the cancers studied so far. Therefore, the levels as well as the activities of the MTA family members are widely accepted as potential biomarkers for diagnosis, prognosis, and predictors of overall survival. They function differently in different cancers with specific mechanisms. p53 and HIF-1α appear to be the respectively common upstream and downstream regulator of the MTA family in both development and metastasis of a wide spectrum of cancers. Here, we review the expression and clinical significance of the MTA family, focusing on hormone-independent cancers. To illustrate the molecular mechanisms, we analyze the MTA family-related signaling pathways in different cancers. Finally, targeting the MTA family directly or the pathways involved in the MTA family indirectly could be invaluable strategies in the development of cancer therapeutics.
Publication Title
Cancer and Metastasis Review
Volume
33
Issue
4
First Page
901
Last Page
919
Recommended Citation
Ning, Zhifeng; Gan, Jinfeng; Chen, Chaoying; Zhang, Dianzheng; and Zhang, Hao, "Molecular Functions and Significance of the MTA Family in Hormone-Independent Cancer" (2014). PCOM Scholarly Works. 384.
https://digitalcommons.pcom.edu/scholarly_papers/384
Comments
This article was published in Cancer Metastasis Review, Volume 33, Issue 4, Pages 901-919.
The published version is available at http://dx.doi.org/10.1007/s10555-014-9517-1.Copyright © 2014 Springer.