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首页> 外文期刊>Nature Communications >Extrapyramidal side effects of antipsychotics are linked to their association kinetics at dopamine D 2 receptors
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Extrapyramidal side effects of antipsychotics are linked to their association kinetics at dopamine D 2 receptors

机译:抗精神病药的锥体束外副作用与其在多巴胺D 2受体上的缔合动力学有关

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摘要

Atypical antipsychotic drugs (APDs) have been hypothesized to show reduced extrapyramidal side effects (EPS) due to their rapid dissociation from the dopamine D2 receptor. However, support for this hypothesis is limited to a relatively small number of observations made across several decades and under different experimental conditions. Here we show that association rates, but not dissociation rates, correlate with EPS. We measured the kinetic binding properties of a series of typical and atypical APDs in a novel time-resolved fluorescence resonance energy transfer assay, and correlated these properties with their EPS and prolactin-elevating liabilities at therapeutic doses. EPS are robustly predicted by a rebinding model that considers the microenvironment of postsynaptic D2 receptors and integrates association and dissociation rates to calculate the net rate of reversal of receptor blockade. Thus, optimizing binding kinetics at the D2 receptor may result in APDs with improved therapeutic profile.
机译:据推测,非典型抗精神病药(APDs)由于其与多巴胺D2受体的快速解离而显示出锥体外系副作用(EPS)减少。但是,对该假设的支持仅限于几十年来在不同实验条件下进行的相对较少的观察结果。在这里,我们显示关联率而不是解离率与EPS相关。我们在新型的时间分辨荧光共振能量转移测定中测量了一系列典型和非典型APD的动力学结合特性,并将这些特性与其在治疗剂量下的EPS和催乳激素升高相关。通过考虑突触后D2受体的微环境并整合缔合和解离速率以计算受体阻滞逆转的净速率的重结合模型,可以强有力地预测EPS。因此,优化D2受体处的结合动力学可以导致具有改善的治疗特性的APD。

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