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在日本肺癌患者中雌激素受体β和芳香化酶的共表达:性别依赖性的临床结局。

Co-expression of estrogen receptor beta and aromatase in Japanese lung cancer patients: gender-dependent clinical outcome.

机构信息

Department of Pathology, Tohoku University School of Medicine, Sendai, Japan.

出版信息

Life Sci. 2012 Oct 22;91(15-16):800-8. doi: 10.1016/j.lfs.2012.08.029. Epub 2012 Sep 6.

DOI:10.1016/j.lfs.2012.08.029
PMID:22982181
Abstract

AIM

The potential gender differences in lung cancer development have been proposed on the basis of hormonal actions. We aimed to evaluate whether estrogen receptors (ERs) in non-small cell carcinoma (NSCLC) patients may primarily depend upon intratumoral estrogen produced via aromatase pathway.

MAIN METHODS

We evaluated ER beta (ERβ) and aromatase status in 169 Japanese NSCLC patients through immunohistochemistry analysis (IHC). Significance of IHC was further confirmed in NSCLC cell lines via in vitro assays.

KEY FINDINGS

IHC analysis of NSCLC patients demonstrated that both ERβ and aromatase were highly co-expressed (p=0.032) in carcinoma cells. Overall survival in males was significantly worse than that in postmenopausal female among double positive NSCLC patients (p=0.010) but not in non-double positive patients. In addition, among double positive cases, overall survival of males was significantly worse than that of postmenopausal females in those with higher ERβ Allred score ≥5, (p=0.034), but not in those with lower ERβ Allred score=3-4. In-vitro analysis demonstrated aromatase activity on testosterone treatment, which resulted in in situ estrogen production (p<0.0001) and increased proliferation of ERβ overexpressing A549 cells (p<0.0001). Aromatase inhibitor i.e. letrozole abrogated this proliferation and also enhanced the androgenic activity (p<0.0001). Testosterone treatment resulted in estrogen responsive elements activation (p<0.0001) in ERβ vector transfected A549 and LK87 cells whereas ER blocker i.e. fulvestrant abrogated this effect, (p<0.0001).

SIGNIFICANCE

Our results suggest that co-expression of ERβ and aromatase in NSCLCs of Japanese males may result in tumor progression and potential endocrine therapy may confer therapeutic benefits to these patients.

摘要

目的

基于激素作用,提出了肺癌发生中潜在的性别差异。我们旨在评估非小细胞癌(NSCLC)患者中的雌激素受体(ER)是否可能主要依赖于芳香酶途径产生的肿瘤内雌激素。

主要方法

我们通过免疫组织化学分析(IHC)评估了 169 名日本 NSCLC 患者的 ERβ(ERβ)和芳香酶状态。通过体外实验进一步确认了 NSCLC 细胞系中 IHC 的意义。

主要发现

对 NSCLC 患者的 IHC 分析表明,ERβ和芳香酶在癌细胞中高度共表达(p=0.032)。在双重阳性 NSCLC 患者中,男性的总生存期明显差于绝经后女性(p=0.010),而非双重阳性患者则无差异。此外,在双重阳性病例中,在 ERβ Allred 评分≥5 的患者中,男性的总生存期明显差于绝经后女性(p=0.034),而在 ERβ Allred 评分=3-4 的患者中则无差异。体外分析表明,芳香酶在睾酮处理时具有活性,导致原位雌激素产生(p<0.0001)和 ERβ过表达 A549 细胞增殖增加(p<0.0001)。芳香酶抑制剂即来曲唑消除了这种增殖作用,并增强了雄激素活性(p<0.0001)。睾酮处理导致 ERβ载体转染的 A549 和 LK87 细胞中的雌激素反应元件激活(p<0.0001),而 ER 阻滞剂即氟维司群则消除了这种作用(p<0.0001)。

意义

我们的结果表明,日本男性 NSCLC 中 ERβ和芳香酶的共表达可能导致肿瘤进展,潜在的内分泌治疗可能为这些患者带来治疗益处。

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