摘要
几十年来,阿片受体一直是治疗疼痛有吸引力的治疗靶点。由于脑啡肽的发现,人们已经知道大约十几个内源性阿片肽可以产生阿片活性和镇痛作用,但他们的治疗方法受到限制,主要是由于低血脑屏障渗透和耐降解性差。一个通用的方法可以克服这些缺点,即针对环肽有限制的结构变化的线性肽环化。相比于它们线性的起源,环状类似物具有更好的代谢稳定性,较低的offtarget毒性,生物利用度的提高。针对有研究前景的化合物的广泛构效关系的研究已经发现用于治疗疼痛以及进一步阐明选择性阿片受体活性所需的结构元素。随之而来的好处是可以通过使用环多环衍生物的生成进一步增强其作用。阿片类药物一般都有短肽链,因此,目前还没有探讨多环肽的领域。在这篇综述中,对阿片受体配体的设计进行了简单的概括,包括经典的线性和环状配体,随着环肽配体的新方法和成功的受体的发展进入了深刻的讨论。阐述和总结了用来提高生物利用度的各种支架和方法,同时对于多环肽也进行了讨论。
关键词: 环肽,多环,阿片受体,镇痛,中枢神经系统,血脑屏障渗透,生物利用度。
Current Medicinal Chemistry
Title:Cyclic Opioid Peptides
Volume: 23 Issue: 13
Author(s): Michael Remesic, Yeon Sun Lee, Victor J. Hruby
Affiliation:
关键词: 环肽,多环,阿片受体,镇痛,中枢神经系统,血脑屏障渗透,生物利用度。
摘要: For decades the opioid receptors have been an attractive therapeutic target for the treatment of pain. Since the first discovery of enkephalin, approximately a dozen endogenous opioid peptides have been known to produce opioid activity and analgesia, but their therapeutics have been limited mainly due to low blood brain barrier penetration and poor resistance to proteolytic degradation. One versatile approach to overcome these drawbacks is the cyclization of linear peptides to cyclic peptides with constrained topographical structure. Compared to their linear parents, cyclic analogs exhibit better metabolic stability, lower offtarget toxicity, and improved bioavailability. Extensive structure-activity relationship studies have uncovered promising compounds for the treatment of pain as well as further elucidate structural elements required for selective opioid receptor activity. The benefits that come with employing cyclization can be further enhanced through the generation of polycyclic derivatives. Opioid ligands generally have a short peptide chain and thus the realm of polycyclic peptides has yet to be explored. In this review, a brief history of designing ligands for the opioid receptors, including classic linear and cyclic ligands, is discussed along with recent approaches and successes of cyclic peptide ligands for the receptors. Various scaffolds and approaches to improve bioavailability are elaborated and concluded with a discourse towards polycyclic peptides.
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Cite this article as:
Michael Remesic, Yeon Sun Lee, Victor J. Hruby , Cyclic Opioid Peptides, Current Medicinal Chemistry 2016; 23 (13) . https://dx.doi.org/10.2174/0929867323666160427123005
DOI https://dx.doi.org/10.2174/0929867323666160427123005 |
Print ISSN 0929-8673 |
Publisher Name Bentham Science Publisher |
Online ISSN 1875-533X |
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