Whitehead T L, McNair S D, Hadden C E, Young J K, Hicks R P
Department of Chemistry, Mississippi State University, Mailstop 9573, Mississippi State, Mississippi 39762, USA.
J Med Chem. 1998 Apr 23;41(9):1497-506. doi: 10.1021/jm970789x.
We present what we believe to be the first documented example of an inducement of distinctly different secondary structure types onto agonists and antagonists selective for the same G-coupled protein receptor using the same membrane-model matrix wherein the induced structures are consistent with those suggested to be biologically active by extensive analogue studies and conventional binding assays. 1H NMR chemical shift assignments for the mammalian NK1 receptor-selective agonists alpha-neurokinin (NKA) and beta-neurokinin (NKB) as well as the mammalian NK1 receptor-selective antagonists [d-Pro2,d-Phe7,d-Trp9]SP and [d-Arg1, d-Pro2,d-Phe7,d-His9]SP have been determined at 600 MHz in sodium dodecyl sulfate (SDS) micelles. The SDS micelle system simulates the membrane-interface environment the peptide experiences when in the proximity of the membrane-embedded receptor, allowing for conformational studies that are a rough approximation of in vivo conditions. Two-dimensional NMR techniques were used to assign proton resonances, and interproton distances were estimated from the observed nuclear Overhauser effects (NOEs). The experimental distances were used as constraints in a molecular dynamics and simulated annealing protocol using the modeling package DISCOVER to generate three-dimensional structures of the two agonists and two antagonists when present in a membrane-model environment to determine possible prebinding ligand conformations. It was determined that (1) NKA is helical from residues 6 to 9, with an extended N-terminus; (2) NKB is helical from residues 4 to 10, with an extended N-terminus; (3) [d-Pro2,d-Phe7,d-Trp9]SP has poorly defined helical properties in the midregion and a beta-turn structure in the C-terminus (residues 6-9); and (4) [d-Arg1,d-Pro2, d-Phe7,d-His9]SP has a helical structure in the midregion (residues 4-6) and a well-defined beta-turn structure in the C-terminus (residues 6-10). Attempts have been made to correlate the observed conformational differences between the agonists and antagonists to their binding potencies and biological activity.
使用相同的膜模型基质,在对同一G偶联蛋白受体具有选择性的激动剂和拮抗剂上诱导出截然不同的二级结构类型,其中诱导结构与通过广泛的类似物研究和传统结合试验表明具有生物活性的结构一致。已在600 MHz下于十二烷基硫酸钠(SDS)胶束中确定了哺乳动物NK1受体选择性激动剂α-神经激肽(NKA)和β-神经激肽(NKB)以及哺乳动物NK1受体选择性拮抗剂[d-Pro2,d-Phe7,d-Trp9]SP和[d-Arg1,d-Pro2,d-Phe7,d-His9]SP的1H NMR化学位移归属。SDS胶束系统模拟了肽在膜嵌入受体附近时所经历的膜界面环境,从而允许进行近似体内条件的构象研究。使用二维NMR技术确定质子共振,并根据观察到的核Overhauser效应(NOE)估计质子间距离。实验距离被用作分子动力学和模拟退火方案中的约束条件,使用建模软件包DISCOVER生成两种激动剂和两种拮抗剂在膜模型环境中的三维结构,以确定可能的预结合配体构象。结果确定:(1)NKA从第6至9位残基呈螺旋结构,N端延伸;(2)NKB从第4至10位残基呈螺旋结构,N端延伸;(3)[d-Pro2,d-Phe7,d-Trp9]SP在中部区域螺旋性质不明确,在C端(第6 - 9位残基)有β-转角结构;(4)[d-Arg1,d-Pro2,d-Phe7,d-His9]SP在中部区域(第4 - 6位残基)有螺旋结构,在C端(第6 - 10位残基)有明确的β-转角结构。已尝试将观察到的激动剂和拮抗剂之间的构象差异与其结合亲和力和生物活性相关联。
