乳腺癌中PR激活形式的肿瘤和细胞分布:一项对大型临床队列的新型免疫组织化学分析
Tumour and cellular distribution of activated forms of PR in breast cancers: a novel immunohistochemical analysis of a large clinical cohort.
作者信息
Bonneterre Jacques, Bosq Jacques, Jamme Philippe, Valent Alexander, Gilles Erard M, Zukiwski Alexander A, Fuqua Suzanne A W, Lange Carol A, O'Shaughnessy Joyce
机构信息
Centre Oscar-Lambret, Université Lille Nord de France , Lille , France.
Institut Gustave Roussy , Villejuif , France.
出版信息
ESMO Open. 2016 Aug 22;1(4):e000072. doi: 10.1136/esmoopen-2016-000072. eCollection 2016.
BACKGROUND
The progesterone receptor (PR) is expressed by ∼70% of early breast tumours and is implicated in the progression of breast cancer. In cancerous tissues PR may be activated in the absence of a ligand, or when ligand concentrations are very low, resulting in aberrantly activated PR (APR). The presence of APR may indicate that patients with breast cancer are more likely to respond to antiprogestins. The aims of this study were to describe and classify the histological subnuclear morphology of active and inactive PR in archival breast cancer samples.
METHODS
Archived tumour specimens from 801 women with invasive breast cancer were collected. Tissue samples (n=789) were analysed for PR isoforms A and B (PRA and PRB), Ki67 and estrogen receptors (ERα) status, using immunohistochemistry. Medical records were used to determine human epidermal growth factor 2 (HER2) status, tumour stage and grade.
RESULTS
A total of 79% of tumours stained positive for either PRA or PRB, and of these 25% of PRA-positive and 23% of PRB-positive tumours had PR present in the activated form. APRA was associated with higher tumour grade (p=0.001). APRB was associated with a higher tumour grade (p=0.046) and a trend for a more advanced stage. Patients with PR-positive tumours treated with antiestrogens had better disease-free survival (DFS) than those with PR-negative tumours (p<0.0001). Cumulative progression rate and DFS were similar irrespective of APR status. Both APRA and APRB were independent of HER2, ERα and Ki67 expression.
CONCLUSIONS
APR had a binary mode of expression in the breast cancer specimens tested, allowing separation into two tumour subsets. APR is an independent target at the cellular and tumour level and may therefore be a suitable predictive marker for antiprogestins, such as onapristone. Using the described technique, a companion diagnostic is under development to identify APR in solid tumours.
背景
约70%的早期乳腺癌组织表达孕激素受体(PR),其与乳腺癌进展有关。在癌组织中,PR可能在无配体存在时或配体浓度极低时被激活,从而导致异常激活的PR(APR)。APR的存在可能表明乳腺癌患者更有可能对抗孕激素产生反应。本研究旨在描述和分类存档乳腺癌样本中活性和非活性PR的组织学亚核形态。
方法
收集801例浸润性乳腺癌女性的存档肿瘤标本。采用免疫组织化学方法对789份组织样本分析PR异构体A和B(PRA和PRB)、Ki67和雌激素受体(ERα)状态。利用病历确定人表皮生长因子2(HER2)状态、肿瘤分期和分级。
结果
共有79%的肿瘤PRA或PRB染色呈阳性,其中25%的PRA阳性肿瘤和23%的PRB阳性肿瘤的PR呈激活形式。APRA与更高的肿瘤分级相关(p=0.001)。APRB与更高的肿瘤分级相关(p=0.046),且有分期更晚的趋势。接受抗雌激素治疗的PR阳性肿瘤患者的无病生存期(DFS)优于PR阴性肿瘤患者(p<0.0001)。无论APR状态如何,累积进展率和DFS相似。APRA和APRB均独立于HER2、ERα和Ki67表达。
结论
在测试的乳腺癌标本中,APR具有二元表达模式,可分为两个肿瘤亚组。APR在细胞和肿瘤水平上是一个独立靶点,因此可能是抗孕激素(如奥那司酮)的合适预测标志物。利用所述技术,正在开发一种伴随诊断方法以识别实体瘤中的APR。
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