The Thyroid Hormone Receptor-RUNX2 Axis: A Novel Tumor Suppressive Pathway in Breast Cancer.

IF 3 4区 医学 Q3 Biochemistry, Genetics and Molecular Biology
Hormones & Cancer Pub Date : 2020-02-01 Epub Date: 2019-12-21 DOI:10.1007/s12672-019-00373-2
Eric L Bolf, Noelle E Gillis, Michael S Barnum, Caitlin M Beaudet, Grace Y Yu, Jennifer A Tomczak, Janet L Stein, Jane B Lian, Gary S Stein, Frances E Carr
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引用次数: 13

Abstract

Metastatic breast cancer is refractory to conventional therapies and is an end-stage disease. RUNX2 is a transcription factor that becomes oncogenic when aberrantly expressed in multiple tumor types, including breast cancer, supporting tumor progression and metastases. Our previous work demonstrated that the thyroid hormone receptor beta (TRβ) inhibits RUNX2 expression and tumorigenic characteristics in thyroid cells. As TRβ is a tumor suppressor, we investigated the compelling question whether TRβ also regulates RUNX2 in breast cancer. The Cancer Genome Atlas indicates that TRβ expression is decreased in the most aggressive basal-like subtype of breast cancer. We established that modulated levels of TRβ results in corresponding changes in the high levels of RUNX2 expression in metastatic, basal-like breast cells. The MDA-MB-231 triple-negative breast cancer cell line exhibits low expression of TRβ and high levels of RUNX2. Increased expression of TRβ decreased RUNX2 levels. The thyroid hormone-mediated suppression of RUNX2 is TRβ specific as TRα overexpression failed to alter RUNX2 expression. Consistent with these findings, knockdown of TRβ in non-tumor MCF10A mammary epithelial-like cells results in an increase in RUNX2 and RUNX2 target genes. Mechanistically, TRβ directly interacts with the proximal promoter of RUNX2 through a thyroid hormone response element to reduce promoter activity. The TRβ suppression of the oncogene RUNX2 is a signaling pathway shared by thyroid and breast cancers. Our findings provide a novel mechanism for TRβ-mediated tumor suppression in breast cancers. This pathway may be common to many solid tumors and impact treatment for metastatic cancers.

甲状腺激素受体runx2轴:乳腺癌中一种新的肿瘤抑制途径。
转移性乳腺癌对常规治疗是难治的,是一种终末期疾病。RUNX2是一种转录因子,当在包括乳腺癌在内的多种肿瘤类型中异常表达时,它就会变成致癌因子,支持肿瘤的进展和转移。我们之前的工作表明,甲状腺激素受体β (TRβ)抑制RUNX2的表达和甲状腺细胞的致瘤特性。由于TRβ是一种肿瘤抑制因子,我们研究了TRβ是否也调节RUNX2在乳腺癌中的作用。癌症基因组图谱显示,TRβ表达在最具侵袭性的基底样乳腺癌亚型中降低。我们证实,TRβ水平的调节导致转移性基底样乳腺细胞中RUNX2高水平表达的相应变化。MDA-MB-231三阴性乳腺癌细胞系TRβ低表达,RUNX2高表达。TRβ表达增加,RUNX2水平降低。甲状腺激素介导的RUNX2的抑制是TRβ特异性的,因为TRα过表达未能改变RUNX2的表达。与这些发现一致,在非肿瘤MCF10A乳腺上皮样细胞中敲低TRβ会导致RUNX2和RUNX2靶基因的增加。从机制上讲,TRβ通过甲状腺激素反应元件直接与RUNX2的近端启动子相互作用以降低启动子活性。TRβ抑制癌基因RUNX2是甲状腺和乳腺癌共有的信号通路。我们的发现为tr β介导的乳腺癌肿瘤抑制提供了一种新的机制。这一途径可能在许多实体肿瘤中是常见的,并影响转移性癌症的治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Hormones & Cancer
Hormones & Cancer ONCOLOGY-ENDOCRINOLOGY & METABOLISM
CiteScore
4.60
自引率
0.00%
发文量
0
期刊介绍: Hormones and Cancer is a unique multidisciplinary translational journal featuring basic science, pre-clinical, epidemiological, and clinical research papers. It covers all aspects of the interface of Endocrinology and Oncology. Thus, the journal covers two main areas of research: Endocrine tumors (benign & malignant tumors of hormone secreting endocrine organs) and the effects of hormones on any type of tumor. We welcome all types of studies related to these fields, but our particular attention is on translational aspects of research. In addition to basic, pre-clinical, and epidemiological studies, we encourage submission of clinical studies including those that comprise small series of tumors in rare endocrine neoplasias and/or negative or confirmatory results provided that they significantly enhance our understanding of endocrine aspects of oncology. The journal does not publish case studies.
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