2014
DOI: 10.1016/j.bmcl.2014.09.029
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Design, synthesis, and structure–activity relationship of novel opioid κ receptor selective agonists: α-Iminoamide derivatives with an azabicyclo[2.2.2]octene skeleton

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Cited by 9 publications
(4 citation statements)
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“…To our notice, NFU elicits its analgesic effects via dual agonistic function at MOR/KOR, while it is also a DOR agonist with a moderate potency. Although some NFU derivatives have been synthesized and reported previously, many of these compounds have not been investigated or reported extensively in biological or pharmacological assays. Taking its clinical success into consideration, NFU is an apparently preferred starting point to explore potential KOR/DOR agonists. Therefore, in the present work, we conducted a complementary structure–activity relationship (SAR) study to systematically understand the multi-opioid receptor pharmacology of NFU analogues in order to reveal potentially valuable information for developing dual KOR/DOR agonists.…”
Section: Introductionmentioning
confidence: 99%
“…To our notice, NFU elicits its analgesic effects via dual agonistic function at MOR/KOR, while it is also a DOR agonist with a moderate potency. Although some NFU derivatives have been synthesized and reported previously, many of these compounds have not been investigated or reported extensively in biological or pharmacological assays. Taking its clinical success into consideration, NFU is an apparently preferred starting point to explore potential KOR/DOR agonists. Therefore, in the present work, we conducted a complementary structure–activity relationship (SAR) study to systematically understand the multi-opioid receptor pharmacology of NFU analogues in order to reveal potentially valuable information for developing dual KOR/DOR agonists.…”
Section: Introductionmentioning
confidence: 99%
“…Several NLF structure–activity relationship (SAR) explorations have been performed and reported. , However, systematic and comprehensive SAR reports on NLF are still missing from literature resources leading to numerous knowledge gaps. , To this end, we recently reported 7 NLF analogues that maintained the same carboxamide side chain at the C 6 -position of the epoxymorphinan skeleton as NLF itself . Herein, we further vary the C 6 -position carboxamide side chain to explore the SAR of this lead with a more robust data set (Figure ).…”
Section: Introductionmentioning
confidence: 99%
“…During the last years a broad range of novel κ agonists belonging to various different structural classes has been reported in the literature. Recently, we have described decahydroquinoxaline κ-opioid receptor agonists representing conformationally restricted analogues of κ agonists U-50,488 ( 2 ) and GR-89,696 ( 3 ). The relative and absolute configuration of decahydroquinoxaline-based κ ligands has a strong impact on their κ affinity. Whereas cis–cis -configured decahydroquinoxaline analogues show very low κ affinity, the trans–trans -configured diasteromer 4 represents a very potent κ agonist ( K i = 9.7 nM).…”
Section: Introductionmentioning
confidence: 99%