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首页> 外文期刊>Journal of biomolecular screening: The official journal of the Society for Biomolecular Screening >Miniaturized receptor binding assays: Complications arising from ligand depletion
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Miniaturized receptor binding assays: Complications arising from ligand depletion

机译:小型化受体结合测定:配体耗竭引起的并发症

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The advent of miniaturized assay formats has made possible the screening of large numbers of compounds against a single target, known as high-throughput screening. Despite this clear advantage, assay miniaturization also increases the risk of ligand depletion, where the actual concentration of free ligand is significantly lower than that added. This, in turn, complicates the interpretation of data from such assays, potentially introducing significant error if not recognized. In this study, the effects of reducing assay volume on radioligand Kd and competitor Ki values have been investigated, using the muscarinic M, receptor as a model system. It was found that assay miniaturization caused dramatic effects, with LIP to a 30-fold underestimation of ligand affinity. A theoretical model was developed and shown to accurately predict both the degree of ligand depletion in any given assay volume and the effect of this depletion on affinity estimates for competing ligands. Importantly, it was found that in most cases, errors introduced by ligand depletion could be largely corrected for by the use of appropriate analysis methods. In addition to those previously described by others, the authors propose a simple method capable of correcting errors in competition binding experiments performed in conditions of ligand depletion.
机译:小型化分析形式的出现使得针对单个靶标筛选大量化合物成为可能,这被称为高通量筛选。尽管具有明显的优势,但测定的小型化也增加了配体耗竭的风险,其中游离配体的实际浓度明显低于所添加的浓度。反过来,这会使来自此类测定法的数据解释变得复杂,如果未识别,可能会引入重大错误。在这项研究中,使用毒蕈碱M1受体作为模型系统,研究了减少测定体积对放射性配体Kd和竞争对手Ki值的影响。发现测定的小型化引起了显着的影响,其中LIP配体亲和力低估了30倍。建立了理论模型并显示出它可以准确预测任何给定测定体积中配体消耗的程度以及这种消耗对竞争性配体亲和力估计的影响。重要的是,发现在大多数情况下,通过使用适当的分析方法,可以很大程度上校正由配体耗尽引起的错误。除了其他人先前描述的方法外,作者还提出了一种简单的方法,该方法能够校正在配体耗尽条件下进行的竞争结合实验中的错误。

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