Department of Molecular Pathology, The Netherlands Cancer Institute, Amsterdam, the Netherlands.
Department of Molecular and Clinical Cancer Medicine, Institute of Translational Medicine, The University of Liverpool, Liverpool, United Kingdom.
Clin Cancer Res. 2016 Jan 15;22(2):479-91. doi: 10.1158/1078-0432.CCR-14-3277. Epub 2015 Sep 14.
The steroid receptor coactivator SRC3 is essential for the transcriptional activity of estrogen receptor α (ERα). SRC3 is sufficient to cause mammary tumorigenesis, and has also been implicated in endocrine resistance. SRC3 is posttranslationally modified by phosphorylation, but these events have not been investigated with regard to functionality or disease association. Here, we investigate the spatial selectivity of SRC3-pS543/DNA binding over the human genome and its expression in primary human breast cancer in relation with outcome.
Chromatin immunoprecipitation, coupled with sequencing, was used to determine the chromatin binding patterns of SRC3-pS543 in the breast cancer cell line MCF7 and two untreated primary breast cancers. IHC was used to assess the expression of SRC3 and SRC3-pS543 in 1,650 primary breast cancers. The relationship between the expression of SRC3 and SRC3-pS543, disease-free survival (DFS), and breast cancer specific survival (BCSS) was assessed.
Although total SRC3 is selectively found at enhancer regions, SRC3-pS543 is recruited to promoters of ERα responsive genes, both in the MCF7 cell line and primary breast tumor specimens. SRC3-pS543 was associated with both improved DFS (P = 0.003) and BCSS (P = 0.001) in tamoxifen untreated high-risk patients, such a correlation was not seen in tamoxifen-treated cases, the interaction was statistically significant (P = 0.001). Multivariate analysis showed SRC3-pS543 to be an independent prognostic factor.
Phosphorylation of SRC3 at S543 affects its genomic interactions on a genome-wide level, where SRC3-pS543 is selectively recruited to promoters of ERα-responsive genes. SRC3-pS543 is a prognostic marker, and a predictive marker of response to endocrine therapy.
类固醇受体共激活因子 SRC3 对于雌激素受体 α(ERα)的转录活性至关重要。SRC3 足以引起乳腺肿瘤的发生,并且还与内分泌抵抗有关。SRC3 可通过磷酸化进行翻译后修饰,但这些事件的功能或与疾病的关联尚未得到研究。在这里,我们研究了 SRC3-pS543/DNA 结合在人类基因组中的空间选择性及其与结局相关的原发性人类乳腺癌中的表达。
使用染色质免疫沉淀结合测序来确定 SRC3-pS543 在乳腺癌细胞系 MCF7 和两个未经处理的原发性乳腺癌中的染色质结合模式。免疫组织化学用于评估 1650 例原发性乳腺癌中 SRC3 和 SRC3-pS543 的表达。评估了 SRC3 和 SRC3-pS543 的表达与无病生存期(DFS)和乳腺癌特异性生存期(BCSS)之间的关系。
尽管总 SRC3 选择性地存在于增强子区域,但 SRC3-pS543 被募集到 ERα 反应基因的启动子,无论是在 MCF7 细胞系还是原发性乳腺癌标本中。SRC3-pS543 与未接受他莫昔芬治疗的高危患者的 DFS(P = 0.003)和 BCSS(P = 0.001)均相关,而在接受他莫昔芬治疗的病例中则未观察到这种相关性,这种相互作用具有统计学意义(P = 0.001)。多变量分析显示 SRC3-pS543 是一个独立的预后因素。
SRC3 在 S543 处的磷酸化影响其在全基因组水平上的基因组相互作用,其中 SRC3-pS543 选择性地募集到 ERα 反应基因的启动子。SRC3-pS543 是一个预后标志物,也是内分泌治疗反应的预测标志物。
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