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枯叶蛱蝶新型 Allatostatin 受体 C 型的配体结合口袋。

Ligand binding pocket of a novel Allatostatin receptor type C of stick insect, Carausius morosus.

机构信息

Boğaziçi University Department of Molecular Biology and Genetics, Istanbul, 34342, Turkey.

Sabancı University Faculty of Engineering and Natural Sciences, Istanbul, 34956, Turkey.

出版信息

Sci Rep. 2017 Jan 24;7:41266. doi: 10.1038/srep41266.

Abstract

Allatostatins (AST) are neuropeptides with variable function ranging from regulation of developmental processes to the feeding behavior in insects. They exert their effects by binding to cognate GPCRs, called Allatostatin receptors (AlstR), which emerge as promising targets for pesticide design. However, AlstRs are rarely studied. This study is the first reported structural study on AlstR-AST interaction. In this work, the first C type AlstR from the stick insect Carausius morosus (CamAlstR-C) was identified and its interaction with type C AST peptide was shown to be physically consistent with the experimental results. The proposed structure of CamAlstR-C revealed a conserved motif within the third extracellular loop, which, together with the N-terminus is essential for ligand binding. In this work, computational studies were combined with molecular and nano-scale approaches in order to introduce an unknown GPCR-ligand system. Consequently, the data obtained provided a reliable target region for future agonist/inverse agonist studies on AlstRs.

摘要

阿特拉托斯汀(AST)是一类具有可变功能的神经肽,其功能范围从调节发育过程到昆虫的摄食行为。它们通过与同源 G 蛋白偶联受体(AlstR)结合发挥作用,AlstR 作为一种有前途的农药设计靶点而备受关注。然而,对 AlstR 的研究却很少。本研究首次报道了 AlstR-AST 相互作用的结构研究。本工作中,首次从 stick insect Carausius morosus 中鉴定出 C 型 AlstR(CamAlstR-C),并证明其与 C 型 AST 肽的相互作用在物理上与实验结果一致。CamAlstR-C 的结构预测揭示了第三个细胞外环内的一个保守基序,该基序连同 N 端对于配体结合是必需的。在这项工作中,计算研究与分子和纳米尺度的方法相结合,以引入一个未知的 GPCR-配体系统。因此,获得的数据为未来 AlstR 的激动剂/反向激动剂研究提供了一个可靠的靶区。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/621c/5259779/3ffd15ff9d8b/srep41266-f1.jpg

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