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灵活性和细胞外开口决定了配体与昆虫速激肽受体之间的相互作用。

Flexibility and extracellular opening determine the interaction between ligands and insect sulfakinin receptors.

作者信息

Yu Na, Zotti Moises João, Scheys Freja, Braz Antônio S K, Penna Pedro H C, Nachman Ronald J, Smagghe Guy

机构信息

Department of Crop Protection, Faculty of Bioscience Engineering, Ghent University, 9000 Ghent, Belgium.

Molecular Entomology and Applied Bioinformatics, Department of Crop Protection, Federal University of Pelotas, 96010-900, Pelotas, RS, Brazil.

出版信息

Sci Rep. 2015 Aug 12;5:12627. doi: 10.1038/srep12627.

Abstract

Despite their fundamental importance for growth, the mechanisms that regulate food intake are poorly understood. Our previous work demonstrated that insect sulfakinin (SK) signaling is involved in inhibiting feeding in an important model and pest insect, the red flour beetle Tribolium castaneum. Because the interaction of SK peptide and SK receptors (SKR) initiates the SK signaling, we have special interest on the structural factors that influence the SK-SKR interaction. First, the three-dimensional structures of the two T. castaneum SKRs (TcSKR1 and TcSKR2) were generated from molecular modeling and they displayed significance in terms of the outer opening of the cavity and protein flexibility. TcSKR1 contained a larger outer opening of the cavity than that in TcSKR2, which allows ligands a deep access into the cavity through cell membrane. Second, normal mode analysis revealed that TcSKR1 was more flexible than TcSKR2 during receptor-ligand interaction. Third, the sulfated SK (sSK) and sSK-related peptides were more potent than the nonsulfated SK, suggesting the importance of the sulfate moiety.

摘要

尽管食物摄入调节机制对于生长至关重要,但其仍未被充分理解。我们之前的研究表明,昆虫速激肽(SK)信号传导参与抑制一种重要的模式害虫——赤拟谷盗的进食。由于SK肽与SK受体(SKR)的相互作用启动了SK信号传导,我们对影响SK - SKR相互作用的结构因素特别感兴趣。首先,通过分子建模生成了两种赤拟谷盗SKR(TcSKR1和TcSKR2)的三维结构,它们在腔的外部开口和蛋白质柔韧性方面具有显著意义。TcSKR1的腔外部开口比TcSKR2的更大,这使得配体能够通过细胞膜深入进入腔内。其次,正常模式分析表明,在受体 - 配体相互作用过程中,TcSKR1比TcSKR2更具柔韧性。第三,硫酸化的SK(sSK)和与sSK相关的肽比非硫酸化的SK更有效,这表明硫酸基团的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/66ae/4542541/6c9b5ba43e8c/srep12627-f1.jpg

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