Solution conformation of mu-selective dermorphin and delta-selective deltorphin-I in phospholipid micelles, studied by NMR spectroscopy and molecular dynamics simulations.

M Segawa, Y Ohno, M Doi, T Ishida, T Iwashita
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Abstract

Complete proton resonance assignments of the naturally occurring mu-selective dermorphin (H-Tyr-D-Ala-Phe-Gly-Tyr-Pro-Ser-NH2) and delta-selective deltorphin-I (H-Tyr-D-Ala-Phe-Asp-Val-Val-Gly-NH2) were carried out by two-dimensional 1H-NMR techniques to investigate the conformational features in the membrane-mimetic micelles of perdeuterated dodecylphosphocholine. Fifty possible three-dimensional structures for respective peptides were generated by means of distance geometry calculations, all of which satisfy the proton-proton distances derived from NOE measurements within the allowable range, and 25 of them were subjected to the molecular dynamics simulations for 10 ps, in which the NOE distances were included as the energetic constraints. Although conformers simulated for dermorphin showed relatively large conformational variations because of the limited NOE data, most of them were characterized as an entirely folded structure bent at the Gly4 residue, where each of the N- and C-terminal tetrapeptides took an extended conformation. On the other hand, most conformations of deltorphin-I showed the common feature that the N-terminal Tyr-D-Ala-Phe-Asp and C-terminal Val-Val-Gly-NH2 sequences took respective folded conformations, and these were almost at right angles on the border of the Asp-Val sequence. These conformational characteristics are discussed in terms of the possible relationship with the mu/delta-opioid receptor selectivity.

用核磁共振波谱和分子动力学模拟研究了多选择性dermorphin和三角洲选择性deltorphin-I在磷脂胶束中的溶液构象。
利用二维核磁共振技术对天然存在的多选择性德尔morphin (h - tyr -d - ala - ph - gly - tyr - pro - ser - nh2)和三角洲选择性德尔海豚- i (h - tyr -d - ala - ph - asp - val - val - gly - nh2)进行了完全质子共振配位,以研究透氘化十二烷基磷胆碱膜模拟胶束的构象特征。通过距离几何计算生成了50种可能的多肽三维结构,它们都满足NOE测量得到的质子-质子距离在允许范围内,并对其中25种进行了10 ps的分子动力学模拟,其中NOE距离作为能量约束。虽然模拟dermorphin的构象由于有限的NOE数据而显示出相对较大的构象变化,但大多数构象的特征是在Gly4残基处弯曲的完全折叠结构,其中每个N端和c端四肽都具有扩展的构象。另一方面,deltorphin-I的大部分构象都表现出n端tyrr - d - ala - phe - asp和c端Val-Val-Gly-NH2序列各自折叠构象的共同特征,且它们在Asp-Val序列的边界上几乎成直角。讨论了这些构象特征与阿片受体选择性的可能关系。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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