Literature DB >> 20032008

The role of oestrogen receptor {alpha} in human thyroid cancer: contributions from coregulatory proteins and the tyrosine kinase receptor HER2.

Dara O Kavanagh1, Marie McIlroy, Eddie Myers, Fiona Bane, Thomas B Crotty, E McDermott, Arnold D Hill, Leonie S Young.   

Abstract

Epidemiological, clinical, and molecular studies suggest a role for oestrogen in thyroid cancer. How oestrogen mediates its effects and the consequence of it on clinical outcome has not been fully elucidated. The participation of coregulatory proteins in modulating oestrogen receptor (ER) function and input of crosstalk with the tyrosine kinase receptor HER2 was investigated. Oestrogen induced cell proliferation in the follicular thyroid cancer (FTC)-133 cells, but not in the anaplastic 8305C cell line. Knockdown of the coactivator steroid receptor coactivator (SRC)-1 inhibited FTC-133 basal, but not oestrogen induced, cell proliferation. Oestrogen also increased protein expression of SRC-1 and the ER target gene cyclin D1 in the FTC-133 cell line. ERalpha, ERbeta, the coregulatory proteins SRC-1 and nuclear corepressor (NCoR), and the tyrosine kinase receptor HER2 were localised by immunohistochemistry and immnofluorescence in paraffin-embedded tissue from thyroid tumour patients (n=111). ERalpha was colocalised with both SRC-1 and NCoR to the nuclei of the tumour epithelial cells. Expression of ERalpha and NCoR was found predominantly in non-anaplastic tumours and was significantly associated with well-differentiated tumours and reduced incidence of disease recurrence. In non-anaplastic tumours, HER2 was significantly associated with SRC-1, and these proteins were associated with poorly differentiated tumours, capsular invasion and disease recurrence. Totally, 87% of anaplastic tumours were positive for SRC-1. Kaplan-Meier estimates of disease-free survival indicated that in thyroid cancer, SRC-1 strongly correlates with reduced disease-free survival (P<0.001), whereas NCoR predicted increased survival (P<0.001). These data suggest opposing roles for the coregulators SRC-1 and NCoR in thyroid tumour progression.

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Year:  2010        PMID: 20032008     DOI: 10.1677/ERC-09-0216

Source DB:  PubMed          Journal:  Endocr Relat Cancer        ISSN: 1351-0088            Impact factor:   5.678


  14 in total

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Authors:  Rehab Allah Ahmed; Engy M Aboelnaga
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6.  Role of estrogen in thyroid function and growth regulation.

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Journal:  J Thyroid Res       Date:  2011-05-04

7.  HER2 Analysis in Sporadic Thyroid Cancer of Follicular Cell Origin.

Authors:  Rosaria M Ruggeri; Alfredo Campennì; Giuseppe Giuffrè; Luca Giovanella; Massimiliano Siracusa; Angela Simone; Giovanni Branca; Rosa Scarfì; Francesco Trimarchi; Antonio Ieni; Giovanni Tuccari
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8.  Immunohistochemical expression of ER-α and PR in papillary thyroid carcinoma.

Authors:  Marwa Mohammed Serag Eldien; Asmaa Gaber Abdou; Tarek Rageh; Eman Abdelrazek; Enas Elkholy
Journal:  Ecancermedicalscience       Date:  2017-06-13

9.  Src-1 and SP2 promote the proliferation and epithelial-mesenchymal transition of nasopharyngeal carcinoma.

Authors:  Jingjing Zhang; Yuanyuan Yang; Hongyu Liu; Hongyi Hu
Journal:  Open Med (Wars)       Date:  2021-07-15

10.  Steroid receptor coactivator-1 interacts with NF-κB to increase VEGFC levels in human thyroid cancer.

Authors:  Bo Gao; Lingji Guo; Donglin Luo; Yan Jiang; Jianjie Zhao; Chengyi Mao; Yan Xu
Journal:  Biosci Rep       Date:  2018-06-12       Impact factor: 3.840

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