2022
DOI: 10.1002/cmdc.202200169
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Opioid Ligands Addressing Unconventional Binding Sites and More Than One Opioid Receptor Subtype

Abstract: Opioid receptors (ORs) represent one of the most significant groups of G‐protein coupled receptor (GPCR) drug targets and also act as prototypical models for GPCR function. In a constant effort to develop drugs with less side effects, and tools to explore the ORs nature and function, various (poly)pharmacological ligand design approaches have been performed. That is, besides classical ligands, a great number of bivalent ligands (i. e. aiming on two distinct OR subtypes), univalent heteromer‐selective ligands a… Show more

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Cited by 7 publications
(9 citation statements)
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“…The dualsteric approach 31 is an emerging pharmacological technique in the past twenty years. Compared to classical orthosteric or allosteric modulators, 15 dualsteric modulators simultaneously bind to orthosteric and allosteric sites.…”
Section: Discussionmentioning
confidence: 99%
See 1 more Smart Citation
“…The dualsteric approach 31 is an emerging pharmacological technique in the past twenty years. Compared to classical orthosteric or allosteric modulators, 15 dualsteric modulators simultaneously bind to orthosteric and allosteric sites.…”
Section: Discussionmentioning
confidence: 99%
“…Firstly, as the mechanism of allosteric drugs is not as direct as orthosteric drugs, so they are usually less potent. [29][30][31] Therefore, it seems hard to simultaneously improve the potency and selectivity in drug design when targeting only one site. Secondly, there is no reason why mutations would not appear in allosteric sites under the selection of drugs.…”
Section: Chengwei Wumentioning
confidence: 99%
“…65,113 In addition, many bivalent ligands aiming at different opioid receptors have been designed and developed. 285 These bivalent ligands consist of two different pharmacophores (agonists or antagonists, connected via a linker) targeting two different receptors. The bivalent ligands targeting KOR can produce similar potential therapeutic benefits to those of mixed KOR agonists while also lacking the typical side effects of pure KOR agonists.…”
Section: Discussionmentioning
confidence: 99%
“…These bivalent ligands consist of two different pharmacophores targeting two different receptors; the two pharmacophores are connected via a linker (also called a spacer). 285 The pharmacophores could be agonists or antagonists of these receptors. 285 For example, KDAN-18 (Figure 9) is a bivalent ligand that targets KOR (agonistic) and DOR (antagonistic) 286 and KMN-21 (Figure 9) is a bivalent ligand that targets KOR (antagonistic) and MOR (antagonistic).…”
Section: Bivalent Kor Ligandsmentioning
confidence: 99%
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