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Screening of 5-HT_(1A) Receptor Antagonists using Molecularly Imprinted Polymers

机译:使用分子印迹聚合物筛选5-HT_(1A)受体拮抗剂

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摘要

Molecular imprinting produces network polymers with recognition sites for imprint molecules. The high binding affinity and selectivity in conjunction with the polymers' physical robustness positions molecular imprinted polymers (MIPs) as candidates for use as preliminary screens in drug discovery. As such, MIPs can serve as crude mimics of native receptors. In an effort to evaluate the relationship between MIPs and native receptors, imprinted polymers for WAY-100635, an antagonist of the serotonin (5-HT) receptor subtype 5-HT_(1A) were prepared. The resulting MIP P(WAY) was evaluated as an affinity matrix in the screening of serotonin receptor antagonists with known affinities for the native receptor. Rough correlations in affinity between the synthetic P(WAY) and native receptor 5-HT_(1A) were found. These findings provide some support for the analogy between MIPs and native receptors and their possible use as surrogates.
机译:分子印迹产生具有印迹分子识别位点的网络聚合物。高结合亲和力和选择性以及聚合物的物理坚固性使分子印迹聚合物(MIP)成为候选药物,可在药物发现中用作初步筛选。这样,MIP可以充当天然受体的粗略模拟物。为了评估MIP与天然受体之间的关系,制备了WAY-100635的印迹聚合物,它是血清素(5-HT)受体亚型5-HT_(1A)的拮抗剂。在筛选对天然受体具有已知亲和力的5-羟色胺受体拮抗剂时,将所得的MIP P(WAY)作为亲和力矩阵进行评估。发现在合成的P(WAY)和天然受体5-HT_(1A)之间的亲和力的粗略相关。这些发现为MIP和天然受体之间的类比及其作为替代物的可能用途提供了支持。

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