Department of Breast Medical Oncology, University of Texas MD Anderson Cancer Center, Houston, TX 77030-4009, USA.
Horm Cancer. 2010 Feb;1(1):21-33. doi: 10.1007/s12672-010-0008-8. Epub 2010 Feb 13.
The trichorhinophalangeal syndrome 1 (TRPS-1) gene is a novel GATA transcription factor family member. Previously, using a gene expression profiling and immunohistochemistry (IHC) screen, we identified TRPS-1 as a highly prevalent gene in breast cancer (BC), expressed in >90% of estrogen receptor alpha (ERα)(+) and ERα(-) BC subtypes. TRPS-1 was also shown to be expressed in prostate cancer where it was shown to play a proapoptotic function during androgen withdrawal possibly through regulating antioxidant metabolism. The role of TRPS-1 and its prognostic significance in hormone-dependent and hormone-independent BC however is not known. In this study, we developed a new quantitative IHC (qIHC) method to further study TRPS-1 as a marker and possible prognostic indicator in BC. By using this method, a quantitative parameter for TRPS-1 expression called a quick score (QS) was derived from the measured labeling index and mean optical density after IHC and applied to a set of 152 stage II/III BC patients from 1993 to 2006 who did not receive preoperative chemotherapy. Associations between QS and tumor characteristics were evaluated using the Kruskal-Wallis test. A wide range of TRPS-1 QS was found among the sample set with higher TRPS-1 QS significantly associated with tumor ERα (p = 0.023 for QS and p = 0.028 for Allred score), progesterone receptor (p = 0.009), and GATA-3 (p < 0.0001). TRPS-1 QS was also positively associated with HER2 status (p = 0.026). Further analysis of different ductal structures in ten BC cases revealed that TRPS-1 expression was expressed at low levels in the remaining normal ducts and in areas of usual ductal hyperplasia but showed marked increase in expression in ductal carcinoma in situ and invasive carcinoma lesions in the tissue. An analysis of TRPS-1 expression in association with overall survival in the 152 stage II/III sample set also revealed that TRPS-1 QS (≥4.0) was significantly associated with improved survival (p = 0.0165). Patients with TRPS-1 QS <4 had a hazard ratio of 2 (p = 0.019) after univariate Cox proportional hazards analysis. In summary, this new qIHC approach was found to reveal critical differences in TRPS-1 expression in primary BC samples and found that it is a promising prognostic marker that should be further evaluated as a possible tumor suppressor gene facilitating improved survival in different subtypes of BC.
三指并趾综合征 1 型 (TRPS-1) 基因是一种新型的 GATA 转录因子家族成员。此前,我们通过基因表达谱和免疫组织化学 (IHC) 筛选,鉴定 TRPS-1 为乳腺癌 (BC) 中高度普遍存在的基因,在>90%的雌激素受体 alpha (ERα)(+)和 ERα(-)BC 亚型中表达。TRPS-1 还在前列腺癌中表达,在雄激素剥夺期间,它可能通过调节抗氧化代谢而发挥促凋亡作用。然而,TRPS-1 在激素依赖性和激素非依赖性 BC 中的作用及其预后意义尚不清楚。在这项研究中,我们开发了一种新的定量 IHC (qIHC) 方法,以进一步研究 TRPS-1 作为 BC 的标志物和可能的预后指标。通过使用这种方法,从 IHC 后的标记指数和平均光密度中得出了一个称为快速评分 (QS) 的 TRPS-1 表达定量参数,并应用于一组 1993 年至 2006 年未接受术前化疗的 152 例 II/III 期 BC 患者。使用 Kruskal-Wallis 检验评估 QS 与肿瘤特征之间的关联。在样本集中发现了广泛的 TRPS-1 QS,较高的 TRPS-1 QS 与肿瘤 ERα(QS 为 p=0.023,Allred 评分 p=0.028)、孕激素受体(p=0.009)和 GATA-3(p<0.0001)显著相关。TRPS-1 QS 与 HER2 状态也呈正相关(p=0.026)。对 10 例 BC 中的不同导管结构的进一步分析表明,TRPS-1 在剩余的正常导管和通常的导管增生区域中低表达,但在导管原位癌和组织中的浸润性癌病变中表达明显增加。对 152 例 II/III 期样本集的 TRPS-1 表达与总生存的关联分析也表明,TRPS-1 QS(≥4.0)与生存改善显著相关(p=0.0165)。单因素 Cox 比例风险分析后,TRPS-1 QS<4 的患者的风险比为 2(p=0.019)。总之,这种新的 qIHC 方法被发现能够揭示原发性 BC 样本中 TRPS-1 表达的关键差异,并发现它是一种很有前途的预后标志物,应进一步评估其作为促进不同 BC 亚型生存改善的可能肿瘤抑制基因。
