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通过¹H-NMR光谱研究局部麻醉药与磷脂酰丝氨酸悬浮液中Na⁺通道失活门肽之间的相互作用。

Interactions between local anesthetics and Na+ channel inactivation gate peptides in phosphatidylserine suspensions as studied by 1H-NMR spectroscopy.

作者信息

Kuroda Y, Miyamoto K, Tanaka K, Maeda Y, Ishikawa J, Hinata R, Otaka A, Fujii N, Nakagawa T

机构信息

Graduate School of Pharmaceutical Sciences, Kyoto University, Japan.

出版信息

Chem Pharm Bull (Tokyo). 2000 Sep;48(9):1293-8. doi: 10.1248/cpb.48.1293.

Abstract

Interactions between local anesthetics and a sodium channel inactivation gate peptide (Ac-GGQDIFMTEEQK-NH2, MP-1A), which was dissected from the cytoplasmic linker between domains III and IV of the sodium channel alpha-subunit (G1484-K1495 in rat brain type IIA), have been studied by 1H-NMR spectroscopy. Changes in 1H-NMR chemical shifts of the aromatic proton resonances of dibucaine (pH 7.0) and lidocaine (pH 6.0 and 9.0) in phosphatidylserine (PS) suspensions were observed. The effects of substitution of glutamine (F1489Q; MP-2A) or D-phenylalanine (MP-1A') for L-phenylalanine (F1489) in MP-1A and the effects of substitution of neutral amino acid residues for the corresponding acidic amino acid residues (D1487N, MP-1NA; E1492Q, MP-IQEA; E1493Q, MP-IEQA) in MP-1A, on the aromatic 1H-NMR chemical shift changes of dibucaine and lidocaine were also investigated. From these results it was concluded that: the aromatic ring of phenylalanine of MP-1A and the aromatic ring of the cationic form of dibucaine or lidocaine are interacting by pi-pi stacking; the tertiary amine nitrogen of dibucaine is interacting electrostatically with D1487, whereas that of lidocaine is interacting with E1492.

摘要

已通过1H-核磁共振光谱研究了局部麻醉药与钠通道失活门控肽(Ac-GGQDIFMTEEQK-NH2,MP-1A)之间的相互作用,该肽段取自钠通道α亚基结构域III和IV之间的胞质连接区(大鼠脑IIA型中的G1484-K1495)。观察到在磷脂酰丝氨酸(PS)悬浮液中,丁卡因(pH 7.0)和利多卡因(pH 6.0和9.0)的芳族质子共振的1H-核磁共振化学位移发生变化。还研究了在MP-1A中用谷氨酰胺(F1489Q;MP-2A)或D-苯丙氨酸(MP-1A')替代L-苯丙氨酸(F1489)的效果,以及在MP-1A中用中性氨基酸残基替代相应酸性氨基酸残基(D1487N,MP-1NA;E1492Q,MP-IQEA;E1493Q,MP-IEQA)对丁卡因和利多卡因芳族1H-核磁共振化学位移变化的影响。从这些结果得出以下结论:MP-1A的苯丙氨酸芳环与丁卡因或利多卡因阳离子形式的芳环通过π-π堆积相互作用;丁卡因的叔胺氮与D1487发生静电相互作用,而利多卡因的叔胺氮与E1492相互作用。

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