Literature DB >> 23015261

Elevated nuclear expression of the SMRT corepressor in breast cancer is associated with earlier tumor recurrence.

Carolyn L Smith1, Ilenia Migliaccio, Vaishali Chaubal, Meng-Fen Wu, Margaret C Pace, Ryan Hartmaier, Shiming Jiang, Dean P Edwards, M Carolina Gutiérrez, Susan G Hilsenbeck, Steffi Oesterreich.   

Abstract

Silencing mediator of retinoic acid and thyroid hormone receptor (SMRT), also known as nuclear corepressor 2 (NCOR2) is a transcriptional corepressor for multiple members of the nuclear receptor superfamily of transcription factors, including estrogen receptor-α (ERα). In the classical model of corepressor action, SMRT binds to antiestrogen-bound ERα at target promoters and represses ERα transcriptional activity and gene expression. Herein SMRT mRNA and protein expression was examined in a panel of 30 breast cancer cell lines. Expression of both parameters was found to vary considerably amongst lines and the correlation between protein and mRNA expression was very poor (R (2) = 0.0775). Therefore, SMRT protein levels were examined by immunohistochemical staining of a tissue microarray of 866 patients with stage I-II breast cancer. Nuclear and cytoplasmic SMRT were scored separately according to the Allred score. The majority of tumors (67 %) were negative for cytoplasmic SMRT, which when detected was found at very low levels. In contrast, nuclear SMRT was broadly detected. There was no significant difference in time to recurrence (TTR) according to SMRT expression levels in the ERα-positive tamoxifen-treated patients (P = 0.297) but the difference was significant in the untreated patients (P = 0.01). In multivariate analysis, ERα-positive tamoxifen-untreated patients with high nuclear SMRT expression (SMRT 5-8, i.e., 2nd to 4th quartile) had a shorter TTR (HR = 1.94, 95 % CI, 1.24-3.04; P = 0.004) while there was no association with SMRT expression for ERα-positive tamoxifen-treated patients. There was no association between SMRT expression and overall survival for patients, regardless of whether they received tamoxifen. Thus while SMRT protein expression was not predictive of outcome after antiestrogen therapy, it may have value in predicting tumor recurrence in patients not receiving adjuvant tamoxifen therapy.

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Year:  2012        PMID: 23015261      PMCID: PMC3511772          DOI: 10.1007/s10549-012-2262-7

Source DB:  PubMed          Journal:  Breast Cancer Res Treat        ISSN: 0167-6806            Impact factor:   4.872


  40 in total

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2.  Expression of nuclear receptor interacting proteins TIF-1, SUG-1, receptor interacting protein 140, and corepressor SMRT in tamoxifen-resistant breast cancer.

Authors:  C M Chan; A E Lykkesfeldt; M G Parker; M Dowsett
Journal:  Clin Cancer Res       Date:  1999-11       Impact factor: 12.531

3.  Cooperative activation of cyclin D1 and progesterone receptor gene expression by the SRC-3 coactivator and SMRT corepressor.

Authors:  Sudipan Karmakar; Tong Gao; Margaret C Pace; Steffi Oesterreich; Carolyn L Smith
Journal:  Mol Endocrinol       Date:  2010-04-14

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Authors:  R K Ross; A Paganini-Hill; P C Wan; M C Pike
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Journal:  J Clin Oncol       Date:  2010-08-09       Impact factor: 44.544

6.  Nuclear IRS-1 predicts tamoxifen response in patients with early breast cancer.

Authors:  Ilenia Migliaccio; Meng-Fen Wu; Carolina Gutierrez; Luca Malorni; Syed K Mohsin; D Craig Allred; Susan G Hilsenbeck; C Kent Osborne; Heidi Weiss; Adrian V Lee
Journal:  Breast Cancer Res Treat       Date:  2009-11-19       Impact factor: 4.872

Review 7.  Normal and cancer-related functions of the p160 steroid receptor co-activator (SRC) family.

Authors:  Jianming Xu; Ray-Chang Wu; Bert W O'Malley
Journal:  Nat Rev Cancer       Date:  2009-09       Impact factor: 60.716

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Authors:  Xiwen Cheng; Hung-Ying Kao
Journal:  J Biol Chem       Date:  2009-10-26       Impact factor: 5.157

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Journal:  Br J Cancer       Date:  2009-11-10       Impact factor: 7.640

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Authors:  Jessica Kao; Keyan Salari; Melanie Bocanegra; Yoon-La Choi; Luc Girard; Jeet Gandhi; Kevin A Kwei; Tina Hernandez-Boussard; Pei Wang; Adi F Gazdar; John D Minna; Jonathan R Pollack
Journal:  PLoS One       Date:  2009-07-03       Impact factor: 3.240
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  9 in total

Review 1.  Minireview: The Link Between ERα Corepressors and Histone Deacetylases in Tamoxifen Resistance in Breast Cancer.

Authors:  Stéphanie Légaré; Mark Basik
Journal:  Mol Endocrinol       Date:  2016-07-20

2.  Activation of p53 transcriptional activity by SMRT: a histone deacetylase 3-independent function of a transcriptional corepressor.

Authors:  Anbu Karani Adikesavan; Sudipan Karmakar; Patricia Pardo; Liguo Wang; Shuang Liu; Wei Li; Carolyn L Smith
Journal:  Mol Cell Biol       Date:  2014-01-21       Impact factor: 4.272

3.  Dual-mechanism estrogen receptor inhibitors.

Authors:  Jian Min; Jerome C Nwachukwu; Charles K Min; Jacqline W Njeri; Sathish Srinivasan; Erumbi S Rangarajan; Charles C Nettles; Valeria Sanabria Guillen; Yvonne Ziegler; Shunchao Yan; Kathryn E Carlson; Yingwei Hou; Sung Hoon Kim; Scott Novick; Bruce D Pascal; Rene Houtman; Patrick R Griffin; Tina Izard; Benita S Katzenellenbogen; John A Katzenellenbogen; Kendall W Nettles
Journal:  Proc Natl Acad Sci U S A       Date:  2021-08-31       Impact factor: 11.205

4.  HP1γ Promotes Lung Adenocarcinoma by Downregulating the Transcription-Repressive Regulators NCOR2 and ZBTB7A.

Authors:  Hunain Alam; Na Li; Shilpa S Dhar; Sarah J Wu; Jie Lv; Kaifu Chen; Elsa R Flores; Laura Baseler; Min Gyu Lee
Journal:  Cancer Res       Date:  2018-05-15       Impact factor: 12.701

5.  The SMRT coregulator enhances growth of estrogen receptor-α-positive breast cancer cells by promotion of cell cycle progression and inhibition of apoptosis.

Authors:  Julia K Blackmore; Sudipan Karmakar; Guowei Gu; Vaishali Chaubal; Liguo Wang; Wei Li; Carolyn L Smith
Journal:  Endocrinology       Date:  2014-06-27       Impact factor: 4.736

6.  Structurally Diverse Histone Deacetylase Photoreactive Probes: Design, Synthesis, and Photolabeling Studies in Live Cells and Tissue.

Authors:  Shaimaa M Aboukhatwa; Thomas W Hanigan; Taha Y Taha; Jayaprakash Neerasa; Rajeev Ranjan; Eman E El-Bastawissy; Mohamed A Elkersh; Tarek F El-Moselhy; Jonna Frasor; Nadim Mahmud; Alan McLachlan; Pavel A Petukhov
Journal:  ChemMedChem       Date:  2019-04-10       Impact factor: 3.540

7.  An integrative transcriptomics approach identifies miR-503 as a candidate master regulator of the estrogen response in MCF-7 breast cancer cells.

Authors:  Jeanette Baran-Gale; Jeremy E Purvis; Praveen Sethupathy
Journal:  RNA       Date:  2016-08-18       Impact factor: 4.942

8.  The pan-cancer lncRNA PLANE regulates an alternative splicing program to promote cancer pathogenesis.

Authors:  Liu Teng; Yu Chen Feng; Su Tang Guo; Pei Lin Wang; Teng Fei Qi; Yi Meng Yue; Shi Xing Wang; Sheng Nan Zhang; Cai Xia Tang; Ting La; Yuan Yuan Zhang; Xiao Hong Zhao; Jin Nan Gao; Li Yuan Wei; Didi Zhang; Jenny Y Wang; Yujie Shi; Xiao Ying Liu; Jin Ming Li; Huixia Cao; Tao Liu; Rick F Thorne; Lei Jin; Feng-Min Shao; Xu Dong Zhang
Journal:  Nat Commun       Date:  2021-06-18       Impact factor: 14.919

9.  The pregnane X receptor (PXR) and the nuclear receptor corepressor 2 (NCoR2) modulate cell growth in head and neck squamous cell carcinoma.

Authors:  Juan Pablo Rigalli; Matthias Reichel; Tasmin Reuter; Guillermo Nicolás Tocchetti; Gerhard Dyckhoff; Christel Herold-Mende; Dirk Theile; Johanna Weiss
Journal:  PLoS One       Date:  2018-02-22       Impact factor: 3.240
  9 in total

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