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A Novel Cellular Model to Study Angiotensin II AT2 Receptor Function in Breast Cancer Cells

机译:研究乳腺癌细胞中血管紧张素II AT2受体功能的新型细胞模型

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Recent studies have highlighted the AT1 receptor as a potential therapeutic target in breast cancer, while the role of the AT2 subtype in this disease has remained largely neglected. The present study describes the generation and characterization of a new cellular model of human invasive breast cancer cells (D3H2LN-AT2) stably expressing high levels of Flag-tagged human AT2 receptor (Flag-hAT2). These cells exhibit high-affinity binding sites for AngII, and total binding can be displaced by the AT2-selective antagonist PD123319 but not by the AT1-selective antagonist losartan. Of interest, high levels of expression of luciferase and green fluorescent protein make these cells suitable for bioluminescence and fluorescence studiesin vitroandin vivo. We provide here a novel tool to investigate the AT2 receptor functions in breast cancer cells, independently of AT1 receptor activation.
机译:最近的研究突出了AT1受体作为乳腺癌的潜在治疗靶标,而AT2亚型在该疾病中的作用仍被很大程度上忽略。本研究描述了稳定表达高水平标记人类AT2受体(Flag-hAT2)的人类浸润性乳腺癌细胞(D3H2LN-AT2)新型细胞模型的生成和表征。这些细胞显示出与AngII的高亲和力结合位点,总结合可以被AT2选择性拮抗剂PD123319取代,而不能被AT1选择性拮抗剂氯沙坦取代。令人感兴趣的是,荧光素酶和绿色荧光蛋白的高水平表达使这些细胞适合于体内外的生物发光和荧光研究。我们在这里提供了一种新颖的工具,可独立于AT1受体激活来研究乳腺癌细胞中的AT2受体功能。

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