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Discovery of the first non-peptide antagonist of the motilin receptor.

机译:发现胃动素受体的第一个非肽拮抗剂。

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A first-in-class non-peptide antagonist of the motilin receptor was identified through electronic screening of our corporate database against a 3D pharmacophore. The pharmacophore was developed from the motilin 22 residue endogenous peptide using NMR structural data, principles of peptide folding, and peptide structure activity relationships. The NMR data supported helical content within the peptide, and both the hydrophobic staple and N-capping box motifs were identified in the motilin sequence. The conformational features of these motifs were imposed on the peptide structure, providing a constrained conformer as a starting point for database searching. A trisubstituted cyclopentene lead was identified directly from the electronic search. Compounds in this series inhibit the binding of 125I-motilin to human antral smooth muscle membrane and antagonize motilin-induced intracellular calcium mobilization in cells expressing the human motilin receptor. A potent compound developed through optimization, RWJ 68023, is active in binding and cell-based functional assays and is also effective in inhibiting motilin-induced contractility in segments of rabbit duodenum. This orally active compound is currently undergoing clinical evaluation for the treatment of gastrointestinal disorders associated with altered motility.
机译:通过针对3D药效团对我们的公司数据库进行电子筛选,鉴定了胃动素受体的一流非肽拮抗剂。使用NMR结构数据,肽折叠原理和肽结构活性关系从胃动素22残基内源肽开发了药效团。 NMR数据支持了肽中的螺旋含量,并且在胃动蛋白序列中鉴定了疏水性钉书钉和N帽盒基序。这些基序的构象特征被施加到肽结构上,提供了受约束的构象异构体作为数据库搜索的起点。直接从电子检索中鉴定出三取代的环戊烯铅。该系列化合物可抑制125I-胃动素与人胃窦平滑肌膜的结合,并在表达人胃动素受体的细胞中拮抗胃动素诱导的细胞内钙动员。通过优化开发的有效化合物RWJ 68023在结合和基于细胞的功能测定中具有活性,并且在抑制十二指肠段中胃动素诱导的收缩性方面也很有效。该口服活性化合物目前正在接受临床评估,以治疗与运动性改变有关的胃肠道疾病。

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