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Downregulated of MTA-3 in ER-negative Breast Tumors

2019.8.03

Approximately 30% of breast carcinomas lack ER expression. Presumably, these breast cancers become estrogen independent through genetic alterations that bypass the requirement for ER-dependent stimulation of cell proliferation. As such estrogen receptor is a key regulator of proliferation and differentiation in mammary epithelia and represents a crucial prognostic indicator and therapeutic target in breast cancer. Mechanistically, estrogen receptor induces changes in gene expression through direct gene activation of a number of genes (cathepsin D, HSP27 (heat shock protein 27,000 kDa, aldolase A, dehydrogenase, alpha-tubulin, and glyceraldehyde-3-phosphat, Pdzk1, Greb ets) and also through the biological functions of target loci. The product of human MTA3 has been identified as an estrogen-dependent component of the Mi-2/NuRD transcriptional corepressor in breast epithelial cells and demonstrate that MTA3 constitutes a key component of an estrogen-dependent pathway regulating growth and differentiation. The absence of estrogen receptor or of MTA3 leads to aberrant expression of the transcriptional repressor Snail, a master regulator of epithelial to mesenchymal transitions. Aberrant Snail expression results in loss of expression of the cell adhesion molecule E-cadherin, an event associated with changes in epithelial architecture and invasive growth. MTA3 is the mechanistic link between estrogen receptor status and invasive growth of breast cancers.

Contributor: Kosi Gramatikoff, PhD

REFERENCES: Bieche I et al. Identification of CGA as a novel estrogen receptor-responsive gene in breast cancer: an outstanding candidate marker to predict the response to endocrine therapy.Cancer Res. 2001 Feb 15;61(4):1652-8. PMID: 11245479 Fujita N et al. MTA3, a Mi-2/NuRD complex subunit, regulates an invasive growth pathway in breast cancer.Cell. 2003 Apr 18;113(2):207-19. PMID: 12705869 Ghosh MG et al. PDZK1 and GREB1 are estrogen-regulated genes expressed in hormone-responsive breast cancer.Cancer Res. 2000 Nov 15;60(22):6367-75. PMID: 11103799 Kumar R. Another tie that binds the MTA family to breast cancer.Cell. 2003 Apr 18;113(2):142-3. Review. PMID: 12705862 Pethe V, Shekhar PV. Estrogen inducibility of c-Ha-ras transcription in breast cancer cells...J Biol Chem. 1999 Oct 22;274(43):30969-78. PMID: 10521493


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