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Design of novel peptide ligands which have opioid agonist activity and CCK antagonist activity for the treatment of pain

机译：具有阿片激动剂活性和CCK拮抗剂活性的新型肽配体的设计用于治疗疼痛

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摘要

Disease states such as neuropathic pain offer special challenges in drug design due to the system changes which accompany these diseases. In this manuscript we provide an example of a new approach to drug design in which we have modified a potent and selective peptide ligand for the CCK-2 receptor to a peptide which has potent agonist binding affinity and bioactivity at delta and mu opioid receptors, and simultaneous antagonist activity at CCK receptors. De novo design based on the concept of overlapping pharmacophores was a central hypothesis of this design, and led to compounds such as H-Tyr-DPhe-Gly-DTrp-NMeNle-Asp-Phe-NH2 (i.e., RSA 601) which have the designed properties.

机译：由于伴随这些疾病的系统变化，诸如神经性疼痛之类的疾病状态在药物设计中提出了特殊的挑战。在本手稿中，我们提供了一种新的药物设计方法的例子，其中我们将CCK-2受体的有效和选择性肽配体修饰为对δ和μ阿片受体具有有效的激动剂结合亲和力和生物活性的肽，并且CCK受体同时具有拮抗剂活性。基于重叠药效团概念的从头设计是该设计的主要假设，并导致了诸如H-Tyr-DPhe-Gly-DTrp-NMeNle-Asp-Phe-NH2（即RSA 601）这样的化合物。设计的属性。

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期刊名称 other
作者
V.J. Hruby; R.S. Agnes; P. Davis; S.-W. Ma; Y.S. Lee; T.W. Vanderah; J. Lai; F. Porreca;
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作者单位

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年(卷),期 -1(73),6
年度 -1
页码 699–704
总页数 9
原文格式 PDF
正文语种
中图分类
关键词
Peptide drug design Opioid agonists Cholecystokinin antagonists Neuropathic pain;

机译：肽类药物设计;阿片类激动剂;胆囊收缩素拮抗剂;神经性疼痛;

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专利

1. Design of novel peptide ligands which have opioid agonist activity and CCK antagonist activity for the treatment of pain. [J] . Hruby VJ, Agnes RS, Davis P, Life sciences . 2003,第6期

机译：具有阿片样物质激动剂活性和CCK拮抗剂活性的新型肽配体的设计，用于治疗疼痛。
2. Design and Synthesis of Novel Hydrazide-Linked Bifunctional Peptides as delta/mu Opioid Receptor Agonists and CCK-l/CCK-2 Receptor Antagonists [J] . Yeon Sun Lee, Richard S.Agnes, Hamid Badghisi, Journal of Medicinal Chemistry . 2006,第5期

机译：新型与酰肼连接的双功能肽δ/μ阿片受体激动剂和CCK-1 / CCK-2受体拮抗剂的设计与合成
3. A bifunctional and peptide-based opioid agonist-nociceptin antagonist ligand for treatment of pain: is the benefit-to-neurorespiratory toxicity ratio improved compared to the usual opioids? [J] . Lagard Camille, Chevillard Lucie, Risede Patricia, Clinical toxicology: the official journal of the American Academy of Clinical Toxicology and European Association of Poisons Centres and Clinical Toxicologists . 2016,第4期

机译：一种用于治疗疼痛的基于肽的双功能类阿片激动剂-伤害受体拮抗剂配体：与普通阿片类药物相比，对神经呼吸系统的毒性比是否有所改善？
4. 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
5. 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。
6. Discovery of Novel Multifunctional Ligands with μ/δ Opioid Agonist/Neurokinin-1 (NK1) Antagonist Activities for the Treatment of Pain [O] . Aswini Kumar Giri, Christopher R. Apostol, Yue Wang, -1

机译：发现具有μ/δ阿片激动剂/神经激肽-1（NK1）拮抗剂活性的新型多功能配体可用于治疗疼痛。
7. Design and Synthesis of Novel Hydrazide-Linked Bifunctional Peptides as d/m Opioid Receptor Agonists and CCK-1/CCK-2 Receptor Antagonists [O] . -1

机译：D / M阿片受体激动剂和CCK-1 / CCK-2受体拮抗剂的设计与合成新的酰肼连接的双官能肽

Design of novel peptide ligands which have opioid agonist activity and CCK antagonist activity for the treatment of pain

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