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首页> 外文期刊>Combinatorial Chemistry _High Throughput Screening >A Directly Labeled TR-FRET Assay for Monitoring Phosphoinositide-3-Kinase Activity
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A Directly Labeled TR-FRET Assay for Monitoring Phosphoinositide-3-Kinase Activity

机译:直接标记的TR-FRET检测用于监测磷酸肌醇3-激酶活性

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摘要

Phosphoinositide 3-kinases (PI3Ks) comprise a family of kinases that transfer the terminal phosphate of adenosine triphosphate to phosphoinositides at the 3-hydroxyl of the inositol ring to form phosphoinositide (3,4,5) triphosphate (PIP3). The PI3Ks have been shown to play key roles in cell growth, motility, morphology, and survival and thus are of interest as targets in anti-inflammatory and anti-oncogenic drug development. To facilitate identification of novel and selective inhibitors of PI3Ks, we have developed a TR-FRET assay that uses directly labeled reagents. The assay makes use of the high affinity binding of phosphoinositides to a Pleckstrin homology (PH) domain in the general receptor for phosphoinositides 1 (Grp1) protein. It monitors PIP3 produced from the enzymatic reaction by measuring its competition with Bodipy®-FL-labeled PIP3 for binding to Terbium chelate-labeled Grp1. By using directly labeled reagents, this assay configuration offers higher sensitivity and faster binding/dissociation kinetics than existing non-radioactive assays, which are critical for competitive assay formats. The assay is homogenous, robust (Z' = 0.88), and simple and, thus, compatible with high throughput screening (HTS) processes.
机译:磷酸肌醇3-激酶(PI3K)包括一类激酶,其将三磷酸腺苷的末端磷酸转移至肌醇环的3-羟基处的磷酸肌醇以形成磷酸三肌醇(3,4,5)三磷酸(PIP3)。已经显示PI3K在细胞生长,运动性,形态和存活中起关键作用,因此作为抗炎和抗癌药开发的靶标是令人感兴趣的。为方便鉴定PI3K的新型和选择性抑制剂,我们开发了使用直接标记试剂的TR-FRET分析法。该测定法利用磷酸肌醇与磷酸肌醇1(Grp1)蛋白通用受体中的Pleckstrin同源性(PH)域的高亲和力结合。它通过测量酶与Bodipy®-FL标记的PIP3与Ter螯合物标记的Grp1结合的竞争性来监测酶促反应产生的PIP3。通过使用直接标记的试剂,与现有的非放射性测定法相比,这种测定法配置具有更高的灵敏度和更快的结合/解离动力学,这对于竞争性测定法形式至关重要。该测定是均一的,稳健的(Z'= 0.88),并且简单,因此可与高通量筛选(HTS)过程兼容。

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