Overexpression of TFAP2C in Invasive Breast Cancer Correlates with a Poorer Response to Anti-hormone Therapy and Reduced Patient Survival

Overview

Journal J Pathol

Specialty Pathology

Date 2008 Oct 1

PMID 18825690

Citations 37

Authors

J M W Gee

J J Eloranta

J C Ibbitt

J F R Robertson

I O Ellis

T Williams

R I Nicholson

H C Hurst

Affiliations

Soon will be listed here.

Abstract

The AP-2gamma transcription factor encoded by the TFAP2C gene is a member of a family of homologous DNA binding proteins that play essential roles during vertebrate embryogenesis but show a restricted pattern of expression in the adult. Elevated expression of the AP-2alpha and AP-2gamma family members has been associated with a number of neoplasms, particularly breast cancer. Here we present an exploratory immunohistochemical study of an archival primary breast tumour series (n = 75) with parallel clinicopathological data using a new, well-characterized antibody to AP-2gamma. Heterogeneous, exclusively nuclear expression of AP-2gamma was found in the epithelial and myoepithelial compartments of normal breast and within tumour epithelial cells. In the breast cancer series, the most notable association was a correlation between elevated levels of AP-2gamma and shortened patient survival (p = 0.0009*). This relationship was also conserved in ER-positive and ErbB2-negative patients; sub-groups generally considered to have a relatively good prognosis. When patient data for survival and duration of treatment response on anti-hormone therapy were examined by multivariate analysis, AP-2gamma was revealed in this study to be an independent predictor of outcome for both survival (p = 0.005) and response to anti-hormone therapy (p = 0.046). Studies using in vitro models confirmed that while tamoxifen response is associated with lower levels of AP-2gamma, acquisition of resistance to this and other anti-hormone measures (eg faslodex or oestrogen deprivation) is associated with high levels of nuclear AP-2gamma. Together these data suggest that elevated tumour AP-2gamma expression can contribute to the failure of cells to growth arrest following anti-hormone treatment and lead to sustained growth and poorer patient outcome.

Citing Articles

Discovery of therapeutic targets in cancer using chromatin accessibility and transcriptomic data.

Forbes A, Xu D, Cohen S, Pancholi P, Khurana E Cell Syst. 2024; 15(9):824-837.e6.

PMID: 39236711 PMC: 11415227. DOI: 10.1016/j.cels.2024.08.004.

Crucial role of the transcription factors family activator protein 2 in cancer: current clue and views.

Jin C, Luo Y, Liang Z, Li X, Kolat D, Zhao L J Transl Med. 2023; 21(1):371.

PMID: 37291585 PMC: 10249218. DOI: 10.1186/s12967-023-04189-1.

TRIM37 Augments AP-2γ Transcriptional Activity and Cellular Localization via K63-linked Ubiquitination to Drive Breast Cancer Progression.

Cui G, Gao Z, Chang S, Narwade N, Chen Y, Poudel B Int J Biol Sci. 2022; 18(11):4316-4328.

PMID: 35864973 PMC: 9295074. DOI: 10.7150/ijbs.69466.

Mutations in Noncoding -Regulatory Elements Reveal Cancer Driver Cistromes in Luminal Breast Cancer.

El Ghamrasni S, Quevedo R, Hawley J, Mazrooei P, Hanna Y, Cirlan I Mol Cancer Res. 2021; 20(1):102-113.

PMID: 34556523 PMC: 9398156. DOI: 10.1158/1541-7786.MCR-21-0471.

Co-expression of transcription factor AP-2beta (TFAP2B) and GATA3 in human mammary epithelial cells with intense, apicobasal immunoreactivity for CK8/18.

Raap M, Gierendt L, Werlein C, Kuehnle E, Kreipe H, Christgen M J Mol Histol. 2021; 52(6):1257-1264.

PMID: 34117603 PMC: 8616868. DOI: 10.1007/s10735-021-09980-2.