Open Access
An androgen receptor mutation in the MDA-MB-453 cell line model of molecular apocrine breast cancer compromises receptor activity
Nicole L. Moore,Grant Buchanan,Jonathan M. Harris,Luke A. Selth,Tina Bianco-Miotto,Adrienne R. Hanson,Stephen N. Birrell,Lisa M. Butler,Theresa E. Hickey,Wayne D. Tilley +9 more
- 01 Aug 2012
48
TL;DR: It is reported that the AR gene in MDA-MB-453 cells contains a G-T transversion in exon 7, resulting in a receptor variant with a glutamine to histidine substitution at amino acid 865 (Q865H) in the ligand binding domain.
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Abstract: Free to read
Recent evidence indicates that the estrogen receptor-a-negative, androgen receptor (AR)- positive molecular apocrine subtype of breast cancer is driven by AR signaling. The MDA-MB-453 cell line is the prototypical model of this breast cancer subtype; its proliferation is stimulated by androgens such as 5a-dihydrotestosterone (DHT) but inhibited by the progestin medroxyprogesterone acetate (MPA) via AR-mediated mechanisms. We report here that the AR gene in MDAMB- 453 cells contains a G-T transversion in exon 7, resulting in a receptor variant with a glutamine to histidine substitution at amino acid 865 (Q865H) in the ligand binding domain. Compared with wild-type AR, the Q865H variant exhibited reduced sensitivity to DHT and MPA in transactivation assays in MDA-MB-453 and PC-3 cells but did not respond to non-androgenic ligands or receptor antagonists. Ligand binding, molecular modeling, mammalian two-hybrid and immunoblot assays revealed effects of the Q865H mutation on ligand dissociation, AR intramolecular interactions, and receptor stability. Microarray expression profiling demonstrated that DHT and MPA regulate distinct transcriptional programs in MDA-MB-453 cells. Gene Set Enrichment Analysis revealed that DHT- but not MPA-regulated genes were associated with estrogen-responsive transcriptomes from MCF-7 cells and the Wnt signaling pathway. These findings suggest that the divergent proliferative responses of MDA-MB-453 cells to DHT and MPA result from the different genetic programs elicited by these two ligands through the AR-Q865H variant. This work highlights the necessity to characterize additional models of molecular apocrine breast cancer to determine the precise role of AR signaling in this breast cancer subtype. Endocrine-Related Cancer (2012) 19 599–613
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Citations
Role of the androgen receptor in breast cancer and preclinical analysis of enzalutamide.
Dawn R. Cochrane,Sebastian Bernales,Britta M. Jacobsen,Diana M. Cittelly,Erin N. Howe,Nicholas C. D'Amato,Nicole S. Spoelstra,Susan M. Edgerton,Annie Jean,Javier Sanchez Guerrero,Francisco Gómez,Satyanarayana Medicherla,Iván E. Alfaro,Emma McCullagh,Paul Jedlicka,Kathleen C. Torkko,Ann D. Thor,Anthony D. Elias,Andrew Asher Protter,Jennifer K. Richer +19 more
TL;DR: This preclinical study supports the initiation of clinical studies evaluating enzalutamide for treatment of AR+ tumors regardless of ER status, since it blocks both androgen- and estrogen- mediated tumor growth.
Androgen receptor inhibits estrogen receptor-A activity and is prognostic in breast cancer
Amelia A. Peters,Grant Buchanan,Carmela Ricciardelli,Tina Bianco-Miotto,Margaret M. Centenera,Jonathan M. Harris,Shalini Jindal,Davendra Segara,Li Jia,Nicole L. Moore,Susan M. Henshall,Stephen N. Birrell,Gerhard A. Coetzee,R. L. Sutherland,Lisa M. Butler,Wayne D. Tilley +15 more
- 01 Jan 2009
TL;DR: In this paper, the balance between estrogen receptor-α (ERα) and androgen receptor (AR) signaling is a critical determinant of growth in the normal and malignant breast.
279
The Androgen Receptor in Breast Cancer.
Pia Giovannelli,Marzia Di Donato,Giovanni Galasso,Erika Di Zazzo,Antonio Bilancio,Antimo Migliaccio +5 more
TL;DR: The putative role of AR in BC is analyzed and emerging therapies based on the use of new agonists or antagonists or inhibitors will be here discussed.
188
Androgen receptor in triple negative breast cancer
TL;DR: It is suggested that the presence of AR in tumour is either benign or predicts better survival and further translational investigations regarding the mechanisms of androgen action in TNBC are required to explain this discrepancy between clinical and basic studies.
138
Androgen Receptor Biology in Triple Negative Breast Cancer: a Case for Classification as AR+ or Quadruple Negative Disease
Valerie N. Barton,Nicholas C. D'Amato,Michael A. Gordon,Jessica L. Christenson,Anthony D. Elias,Jennifer K. Richer +5 more
TL;DR: It is proposed that TNBC be further sub-classified as either AR+ TNBC or quadruple negative breast cancer since targeting AR may represent a viable therapeutic option for a subset of TNBC.
References
Controlling the false discovery rate: a practical and powerful approach to multiple testing
Yoav Benjamini,Yosef Hochberg +1 more
TL;DR: In this paper, a different approach to problems of multiple significance testing is presented, which calls for controlling the expected proportion of falsely rejected hypotheses -the false discovery rate, which is equivalent to the FWER when all hypotheses are true but is smaller otherwise.
Gene set enrichment analysis: A knowledge-based approach for interpreting genome-wide expression profiles
Aravind Subramanian,Pablo Tamayo,Vamsi K. Mootha,Sayan Mukherjee,Benjamin L. Ebert,Michael A. Gillette,Amanda G. Paulovich,Scott L. Pomeroy,Todd R. Golub,Eric S. Lander,Jill P. Mesirov +10 more
TL;DR: The Gene Set Enrichment Analysis (GSEA) method as discussed by the authors focuses on gene sets, that is, groups of genes that share common biological function, chromosomal location, or regulation.
MOLSCRIPT: a program to produce both detailed and schematic plots of protein structures
TL;DR: The MOLSCRIPT program as discussed by the authors produces plots of protein structures using several different kinds of representations, including simple wire models, ball-and-stick models, CPK models and text labels.
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TL;DR: Gen expression profiles from 21 breast cancer data sets and identified 587 TNBC cases may be useful in biomarker selection, drug discovery, and clinical trial design that will enable alignment of TNBC patients to appropriate targeted therapies.
Raster3D Version 2.0. A program for photorealistic molecular graphics.
TL;DR: Raster3D Version 2.0 is a program suite for the production of photorealistic molecular graphics images, and is particularly suited for use in producing large raster images of macromolecules for output to a film recorder or high-quality color printer.
2.5K