原发性肿瘤中芳香化酶的原位表达与雌激素受体表达相关,但不能预测晚期乳腺癌内分泌治疗的反应。
In situ aromatase expression in primary tumor is associated with estrogen receptor expression but is not predictive of response to endocrine therapy in advanced breast cancer.
作者信息
Lykkesfeldt Anne E, Henriksen Katrine L, Rasmussen Birgitte B, Sasano Hironobu, Evans Dean B, Møller Susanne, Ejlertsen Bent, Mouridsen Henning T
机构信息
Department of Tumor Endocrinology, Institute of Cancer Biology, Danish Cancer Society, Copenhagen Ø, Denmark.
出版信息
BMC Cancer. 2009 Jun 16;9:185. doi: 10.1186/1471-2407-9-185.
BACKGROUND
New, third-generation aromatase inhibitors (AIs) have proven comparable or superior to the anti-estrogen tamoxifen for treatment of estrogen receptor (ER) and/or progesterone receptor (PR) positive breast cancer. AIs suppress total body and intratumoral estrogen levels. It is unclear whether in situ carcinoma cell aromatization is the primary source of estrogen production for tumor growth and whether the aromatase expression is predictive of response to endocrine therapy. Due to methodological difficulties in the determination of the aromatase protein, COX-2, an enzyme involved in the synthesis of aromatase, has been suggested as a surrogate marker for aromatase expression.
METHODS
Primary tumor material was retrospectively collected from 88 patients who participated in a randomized clinical trial comparing the AI letrozole to the anti-estrogen tamoxifen for first-line treatment of advanced breast cancer. Semi-quantitative immunohistochemical (IHC) analysis was performed for ER, PR, COX-2 and aromatase using Tissue Microarrays (TMAs). Aromatase was also analyzed using whole sections (WS). Kappa analysis was applied to compare association of protein expression levels. Univariate Wilcoxon analysis and the Cox-analysis were performed to evaluate time to progression (TTP) in relation to marker expression.
RESULTS
Aromatase expression was associated with ER, but not with PR or COX-2 expression in carcinoma cells. Measurements of aromatase in WS were not comparable to results from TMAs. Expression of COX-2 and aromatase did not predict response to endocrine therapy. Aromatase in combination with high PR expression may select letrozole treated patients with a longer TTP.
CONCLUSION
TMAs are not suitable for IHC analysis of in situ aromatase expression and we did not find COX-2 expression in carcinoma cells to be a surrogate marker for aromatase. In situ aromatase expression in tumor cells is associated with ER expression and may thus point towards good prognosis. Aromatase expression in cancer cells is not predictive of response to endocrine therapy, indicating that in situ estrogen synthesis may not be the major source of intratumoral estrogen. However, aromatase expression in combination with high PR expression may select letrozole treated patients with longer TTP.
TRIAL REGISTRATION
Sub-study of trial P025 for advanced breast cancer.
背景
新型第三代芳香化酶抑制剂(AIs)已被证明在治疗雌激素受体(ER)和/或孕激素受体(PR)阳性乳腺癌方面与抗雌激素他莫昔芬相当或更具优势。AIs可抑制全身和肿瘤内雌激素水平。目前尚不清楚原位癌细胞芳香化是否是肿瘤生长雌激素产生的主要来源,以及芳香化酶表达是否可预测内分泌治疗反应。由于在测定芳香化酶蛋白方面存在方法学困难,参与芳香化酶合成的酶COX-2已被建议作为芳香化酶表达的替代标志物。
方法
回顾性收集了88例参与一项随机临床试验的患者的原发性肿瘤材料,该试验比较了AI来曲唑与抗雌激素他莫昔芬用于晚期乳腺癌一线治疗的疗效。使用组织微阵列(TMAs)对ER、PR、COX-2和芳香化酶进行半定量免疫组织化学(IHC)分析。还使用全切片(WS)对芳香化酶进行分析。应用kappa分析比较蛋白表达水平的相关性。进行单因素Wilcoxon分析和Cox分析以评估与标志物表达相关的进展时间(TTP)。
结果
癌细胞中芳香化酶表达与ER相关,但与PR或COX-2表达无关。WS中芳香化酶的测量结果与TMAs的结果不可比。COX-2和芳香化酶的表达不能预测内分泌治疗反应。芳香化酶与高PR表达联合可能会筛选出来曲唑治疗后TTP较长的患者。
结论
TMAs不适用于原位芳香化酶表达的IHC分析,我们未发现癌细胞中COX-2表达是芳香化酶的替代标志物。肿瘤细胞中原位芳香化酶表达与ER表达相关,因此可能预示预后良好。癌细胞中芳香化酶表达不能预测内分泌治疗反应,表明原位雌激素合成可能不是肿瘤内雌激素的主要来源。然而,芳香化酶表达与高PR表达联合可能会筛选出来曲唑治疗后TTP较长的患者。
试验注册
晚期乳腺癌试验P025的子研究。
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