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多巴胺受体-1(D1R)在乳腺癌中的表达及治疗靶点研究

Expression and therapeutic targeting of dopamine receptor-1 (D1R) in breast cancer.

作者信息

Borcherding D C, Tong W, Hugo E R, Barnard D F, Fox S, LaSance K, Shaughnessy E, Ben-Jonathan N

机构信息

Department of Cancer Biology, University of Cincinnati, Cincinnati, OH, USA.

Department of Pathology, University of Cincinnati, Cincinnati, OH, USA.

出版信息

Oncogene. 2016 Jun 16;35(24):3103-13. doi: 10.1038/onc.2015.369. Epub 2015 Oct 19.

Abstract

Patients with advanced breast cancer often fail to respond to treatment, creating a need to develop novel biomarkers and effective therapeutics. Dopamine (DA) is a catecholamine that binds to five G protein-coupled receptors. We discovered expression of DA type-1 receptors (D1Rs) in breast cancer, thereby identifying these receptors as novel therapeutic targets in this disease. Strong to moderate immunoreactive D1R expression was found in 30% of 751 primary breast carcinomas, and was associated with larger tumors, higher tumor grades, node metastasis and shorter patient survival. DA and D1R agonists, signaling through the cGMP/protein kinase G (PKG) pathway, suppressed cell viability, inhibited invasion and induced apoptosis in multiple breast cancer cell lines. Fenoldopam, a peripheral D1R agonist that does not penetrate the brain, dramatically suppressed tumor growth in two mouse models with D1R-expressing xenografts by increasing both necrosis and apoptosis. D1R-expressing primary tumors and metastases in mice were detected by fluorescence imaging. In conclusion, D1R overexpression is associated with advanced breast cancer and poor prognosis. Activation of the D1R/cGMP/PKG pathway induces apoptosis in vitro and causes tumor shrinkage in vivo. Fenoldopam, which is FDA (Food and Drug Administration) approved to treat renal hypertension, could be repurposed as a novel therapeutic agent for patients with D1R-expressing tumors.

摘要

晚期乳腺癌患者往往对治疗无反应,因此需要开发新的生物标志物和有效的治疗方法。多巴胺(DA)是一种儿茶酚胺,可与五种G蛋白偶联受体结合。我们发现乳腺癌中存在DA 1型受体(D1R)的表达,从而将这些受体确定为该疾病的新治疗靶点。在751例原发性乳腺癌中,30%发现有强至中度免疫反应性D1R表达,且与肿瘤较大、肿瘤分级较高、淋巴结转移及患者生存期较短相关。DA和D1R激动剂通过cGMP/蛋白激酶G(PKG)途径发出信号,可抑制多种乳腺癌细胞系的细胞活力、侵袭并诱导凋亡。非诺多泮是一种不穿透大脑的外周D1R激动剂,通过增加坏死和凋亡,显著抑制了两种表达D1R的异种移植小鼠模型中的肿瘤生长。通过荧光成像检测小鼠中表达D1R的原发性肿瘤和转移灶。总之,D1R过表达与晚期乳腺癌及不良预后相关。激活D1R/cGMP/PKG途径可在体外诱导凋亡并在体内使肿瘤缩小。非诺多泮已获美国食品药品监督管理局(FDA)批准用于治疗肾性高血压,可重新用作治疗表达D1R肿瘤患者的新型治疗药物。

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