Rational drug design and synthesis of a selective opioid receptor antagonist on the basis of the accessory site concept.

Fujii H; Narita M; Mizoguchi H; Hirokawa J; Kawai K; Tanaka T; Tseng LF; Nagase H

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Rational drug design and synthesis of a selective opioid receptor antagonist on the basis of the accessory site concept.

机译：在辅助部位概念的基础上进行合理的药物设计和选择性阿片受体拮抗剂的合成。

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To newly synthesize a selective opioid receptor antagonist, 17-(cyclopropylmethyl)-4,5 alpha-epoxy-6 beta,21-epoxymethano-3-hydroxy-6,14-endoethenomorphinan-7 alpha-(N-phenethyl)carboxamide was first designed from an opioid receptor agonist TAN-821 on the basis of the accessory site concept. The designed compound antagonized the agonistic effects induced by an opioid receptor agonist beta-endorphin on the rat vas deference test. Moreover, the designed compound blocked the antinociception induced by beta-endorphin given intracerebroventricularly.

机译：为了重新合成选择性阿片受体拮抗剂，首先是17-（环丙基甲基）-4,5α-环氧-6β，21-环氧甲氧基-3-羟基-6,14-内啡肽吗啡喃7α-（N-苯乙基）羧酰胺由阿片受体激动剂TAN-821根据辅助部位概念设计而成。所设计的化合物拮抗阿片受体激动剂β-内啡肽对大鼠输卵管基准试验的激动作用。而且，所设计的化合物阻断了由脑室内给予的β-内啡肽诱导的抗伤害感受。

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来源
《Bioorganic and Medicinal Chemistry Letters》 |2004年第16期|共3页
作者
Fujii H; Narita M; Mizoguchi H; Hirokawa J; Kawai K; Tanaka T; Tseng LF; Nagase H;
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原文格式 PDF
正文语种 eng
中图分类基础医学;
关键词
Receptors; Opioid; concept; Drug Design; beta-Endorphin; 受体; 阿片样; 药物设计; β内啡肽;

机译：Receptors;Opioid;concept;Drug Design;beta-Endorphin;受体;阿片样;药物设计;β内啡肽;

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2. Rational drug design and synthesis of a selective opioid receptor antagonist on the basis of the accessory site concept. [J] . Fujii H, Narita M, Mizoguchi H, Bioorganic and Medicinal Chemistry Letters . 2004,第16期

机译：在辅助部位概念的基础上进行合理的药物设计和选择性阿片受体拮抗剂的合成。
3. Rational drug design of selective epsilon opioid receptor agonist TAN-821 and antagonist TAN-1014. [J] . Fujii H, Nagase H Current medicinal chemistry . 2006,第10期

机译：选择性ε类阿片受体激动剂TAN-821和拮抗剂TAN-1014的合理药物设计。
4. Rational Drug Design of Selective ℇ Opioid Receptor Agonist TAN-821 and Antagonist TAN-1014 [J] . H. Fujii H. Nagase Current Medicinal Chemistry . 2006,第10期

机译：选择性ℇ类阿片受体激动剂TAN-821和拮抗剂TAN-1014的合理药物设计
5. Design and synthesis of bifunctional peptides:antagonists at CCKA/CCKB receptors and agonists as mu/delta opioid receptors [C] . Richard S.Agnes, Yeon Sun Lee, Peg Davis, the International Peptide Symposium . 2001

机译：双官能肽的设计与合成：Ccka / Cckb受体的拮抗剂和穆/δ阿片受体的激动剂
6. New paradigm for drug design: Design and synthesis of novel biologically active peptides that are agonists at opioid receptors and antagonists at cholecystokinin receptors. [D] . Agnes, Richard Sario. 2003

机译：药物设计的新范例：设计和合成新型的生物活性肽，这些肽是阿片受体的激动剂，胆囊收缩素受体的拮抗剂。
7. Conformationally Homogeneous Heterocyclic Pseudo-Tetrapeptides as Three-Dimensional Scaffolds for Rational Drug Design: Mapping the Structural Basis Set and Application to the Design of Receptor-Selective Somatostatin Analogues [O] . Mr. John M. Beierle, Dr. W. Seth Horne, Prof. Dr. Jan H. van Maarseveen, -1

机译：构象均一的杂环伪四肽作为三维支架用于合理的药物设计：映射结构基础集并将其应用于受体选择性生长抑素类似物的设计
8. New paradigm for drug design: Design and synthesis of novel biologically active peptides that are agonists at opioid receptors and antagonists at cholecystokinin receptors [O] . Agnes Richard S 2003

机译：药物设计的新范例：设计和合成新型生物活性肽，这些肽是阿片样物质受体的激动剂，而胆囊收缩素受体的拮抗剂

Rational drug design and synthesis of a selective opioid receptor antagonist on the basis of the accessory site concept.

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