Application of phosphorylation site-specific antibodies to measure nuclear receptor signaling: characterization of novel phosphoantibodies for estrogen receptor alpha.

Nuclear receptor signaling Pub Date : 2006-01-01 Epub Date: 2006-04-28 DOI:10.1621/nrs.04007
Mariam H Al-Dhaheri, Brian G Rowan
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引用次数: 32

Abstract

An understanding of posttranslational events in nuclear receptor signaling is crucial for drug design and clinical therapeutic strategies. Phosphorylation is a well-characterized posttranslational modification that regulates subcellular localization and function of nuclear receptors and coregulators. Although the role of single phosphorylation sites in nuclear receptor function has been described, the contribution of combinations of multiple phosphorylation sites to receptor function remains unclear. The development of phosphoantibodies to each phosphorylation site in a nuclear receptor is a powerful tool to address the role of phosphorylation in multiply phosphorylated receptors. However, phosphoantibodies must be rigorously validated prior to use. This review describes the general methodology for design, characterization and validation of phosphoantibodies using the example of eight phosphoantibodies raised against phosphorylation sites in estrogen receptor alpha (ERalpha).

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应用磷酸化位点特异性抗体测量核受体信号:雌激素受体α的新型磷酸化抗体的表征。
了解核受体信号转译后事件对药物设计和临床治疗策略至关重要。磷酸化是一种具有良好特征的翻译后修饰,可调节亚细胞定位和核受体和共调节因子的功能。尽管单个磷酸化位点在核受体功能中的作用已被描述,但多个磷酸化位点的组合对受体功能的贡献仍不清楚。针对核受体中每个磷酸化位点的磷酸化抗体的开发是解决磷酸化在多重磷酸化受体中的作用的有力工具。然而,使用前必须严格验证磷抗体。本文以针对雌激素受体α (erα)磷酸化位点的8种磷酸化抗体为例,描述了设计、表征和验证磷酸化抗体的一般方法。
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