Differential stereochemical requirements of mu vs. delta opioid receptors for ligand binding and signal transduction: development of a class of potent and highly delta-selective peptide antagonists.

机译：mu与delta类阿片受体对配体结合和信号转导的不同立体化学要求：一类有效且高度delta选择性的肽拮抗剂的开发。

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Opioid peptide analogs consisting entirely of aromatic amino acid residues and containing conformationally restricted phenylalanine derivatives in position 2 of the peptide sequence were synthesized and pharmacologically characterized in vitro. Both diastereoisomers of H-Tyr-(D or L)-NMePhe-Phe-Phe-NH2 (NMePhe is N alpha-methylphenylalanine) were mu-receptor-selective, were full agonists in the mu-receptor-representative guinea pig ileum assay, and were partial agonists in the mouse vas deferens assay, with the L-NMePhe2 analog displaying somewhat higher intrinsic activity than the D-NMePhe2 analog. Further conformational restriction at position 2 in the sequence, as achieved through substitution of D- or L-tetrahydro-3-isoquinoline carboxylic acid (Tic), produced a configuration-dependent differential effect on receptor selectivity and intrinsic activity, leading to a potent mu-selective mu agonist (the D-Tic2 analog) with increased intrinsic activity in the mouse vas deferens assay and to a potent delta-selective delta antagonist (the L-Tic2 analog). These results demonstrate that imposition of conformational constraints in a peptide not only may alter receptor selectivity but also may decrease, totally abolish, or even enhance intrinsic activity. The tetrapeptide H-Tyr-Tic-Phe-Phe-NH2 was a moderately potent full agonist in the guinea pig ileum assay and, thus, represents a compound with mixed mu-agonist/delta-antagonist properties. The corresponding peptide with a free C-terminal carboxyl group H-Tyr-Tic-Phe-Phe-OH showed high delta-receptor affinity (Ki delta = 1.2 nM), unprecedented delta selectivity (Ki mu/Ki delta = 1410), high potency as delta antagonist (Ke = 3-8 nM against various delta agonists in the mouse vas deferens assay) and, unlike other delta antagonists, had no mu-antagonist properties. The tripeptides H-Tyr-Tic-Phe-OH and H-Tyr-Tic-Phe-NH2 were also delta antagonists.

机译：合成了完全由芳族氨基酸残基组成且在肽序列第2位含有构象受限的苯丙氨酸衍生物的阿片肽类似物，并在体外进行了药理学表征。 H-Tyr-（D或L）-NMePhe-Phe-Phe-NH2（NMePhe是Nα-甲基苯基丙氨酸）的两种非对映异构体均具有mu受体选择性，在以mu受体代表的豚鼠回肠测定中为完全激动剂，在小鼠输精管试验中是部分激动剂，L-NMePhe2类似物显示出比D-NMePhe2类似物更高的固有活性。通过取代D-或L-四氢-3-异喹啉羧酸（Tic）实现的在序列2位的进一步构象限制，对受体选择性和内在活性产生依赖于构型的差异作用，从而导致有效的mu -选择性μ激动剂（D-Tic2类似物）在小鼠输精管试验中具有增强的内在活性，并具有有效的δ-选择性δ拮抗剂（L-Tic2类似物）。这些结果表明，在肽中构象约束的施加不仅可以改变受体的选择性，而且可以降低，完全消除甚至增强内在活性。在豚鼠回肠测定中，四肽H-Tyr-Tic-Phe-Phe-Phe-NH2是中等效力的完全激动剂，因此代表具有混合的mu-激动剂/δ-拮抗剂特性的化合物。具有游离C末端羧基H-Tyr-Tic-Phe-Phe-OH的相应肽显示出高的delta-受体亲和力（Ki delta = 1.2 nM），空前的delta选择性（Ki mu / Ki delta = 1410），高作为δ拮抗剂的效价（Ke = 3-8 nM，对小鼠输精管试验中的各种δ激动剂而言），并且与其他δ拮抗剂不同，它没有mu拮抗剂特性。三肽H-Tyr-Tic-Phe-OH和H-Tyr-Tic-Phe-NH2也是δ拮抗剂。

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期刊名称 Proceedings of the National Academy of Sciences of the United States of America
作者
P W Schiller; T M Nguyen; G Weltrowska; B C Wilkes; B J Marsden; C Lemieux; N N Chung;
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年(卷),期 1992(89),24
年度 1992
页码 11871–11875
总页数 5
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1. Intracerebroventricular administration of CYX-6, a potent mu-opioid receptor agonist, a delta- and kappa-opioid receptor antagonist and a biased ligand at mu, delta & kappa-opioid receptors, evokes antinociception with minimal constipation and respiratory depression in rats in contrast to morphine [J] . European Journal of Pharmacology: An International Journal . 2020,第期

机译：Cyx-6，富含官能蛋白质受体激动剂，δ和κ-阿片受体受体拮抗剂和静脉δ和κ-阿片类药物受体的偏向配体的脑内腔内施用，唤起抗妇女的大鼠血液化和呼吸抑郁症相反对吗啡
2. Conversion of delta-, kappa- and mu-receptor selective opioid peptide agonists into delta-, kappa- and mu-selective antagonists. [J] . Schiller PW, Weltrowska G, Nguyen TM, Life sciences . 2003,第6期

机译：将δ，κ和μ受体选择性阿片肽激动剂转化为δ，κ和μ选择性拮抗剂。
3. DAMGO, a μ‐opioid receptor selective ligand, distinguishes between μ‐and κ‐opioid receptors at a different region from that for the distinction between μ‐ and δ‐opioid receptors [J] . Aoki Yasuhide, Katao Yoshikazu, Katsumata Seishi, FEBS Letters . 1995,第1期

机译：DAMGO是一种μ阿片受体选择性配体，可区分位于不同区域的μ阿片受体和κ阿片受体，而不同于区分μ阿片和δ阿片受体的区域。
4. Opioid Ligand Binding to Opioid Receptors: Insight and Implications for Peptide Design [C] . Michael J. Ferracane, Jane V. Aldrich American Peptide Symposium . 2015

机译：阿片类配体与阿片受体的结合：肽设计的见解和影响
5. The Design, Synthesis, and Pharmacological Evaluation of Bifunctional Mu-/Delta-Selective Opioid Receptor Ligands for the Treatment of Pain [D] . Nastase, Anthony F. 2018

机译：双官能Mu-/ Delta-Selectience ApiOID受体配体的设计，合成和药理学评估治疗疼痛
6. Synthesis and Opioid Receptor Binding Affinities of 2-Substituted and 3-Aminomorphinans: Ligands for mu kappa and delta Opioid Receptors [O] . Michael Decker, Yu-Gui Si, Brian I. Knapp, -1

机译：合成与阿片受体结合的亲和力2-取代和3- aminomorphinans：配体为μκ和δ阿片受体
7. Differential stereochemical requirements of mu vs. delta opioid receptors for ligand binding and signal transduction: development of a class of potent and highly delta-selective peptide antagonists. [O] . Schiller, P W, Nguyen, T M, Weltrowska, G, 1992

机译：mu与delta类阿片受体对配体结合和信号转导的不同立体化学要求：一类有效且高度delta选择性的肽拮抗剂的开发。

Differential stereochemical requirements of mu vs. delta opioid receptors for ligand binding and signal transduction: development of a class of potent and highly delta-selective peptide antagonists.

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