4DQSAR
Bluelighter
- Joined
- Feb 3, 2025
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I was taking a quick look at 3-(dimethylamino)-2,2-dimethyl-1-phenylpropan-1-one. I discovered that the para fluoro and para chloro derivatives had been made and their analgesic activity tested.
So we have at least a little more QSAR data.
Original paper: 'Analgetics. II. Relationship between structure and activity of some beta-amino ketones'
Paper in which para halo derivatives are tested: 'β-Amino Ketones. Synthesis and Some Biological Activities in mice of 3,3-Dialkyl-1,2,3,4-tetrahydro-4-quinolinones and Related Mannich Bases'
H - 16mg/Kg
F - 45mg/kg
Cl - 85 mg/kg
Like all good research, a negative result is still a valid and useful result.
What REALLY astounds me is that while the original paper does include some ring-substituted examples, it only covers ortho hydroxy and para methoxy examples. The meta hydroxy is not explored.
A further search revealed a rigid analogue which WAS an opioid AGONIST (and important detail as affinity ≠ effacacy) in the papers:
Opioid agonist and antagonist effects of configurational stereoisomers of 3-(dimethylamino)-2,2-dimethyl-7-hydroxy-1-tetralol
Opioid receptor effects of two 3-amino-2,2-dimethyltetralin analogs in guinea pig ileum longitudinal muscle
Opioid receptor effects of two aminotetralin derivatives using the electrically driven mouse vas deferens
But I was unable to locate ANY of the above papers (anyone?). The tetralin being phenolic and chiral revealed what is quite common. One enantiomer being an agonist, the other an antagonist.
I think most people have missed the fact that the simple, weak opioid discovered in the 1960s is closely related to the much more potent (3R)-2,2-dimethyl-3-(dimethylamino)-3-phenyl-N-(2-phenylethyl)propanamide class which itself overlays BDPC and ciramadol. In that case the phenolic derivatives are far more potent BUT the raecemates at least are antagonists. The KEY breaktrhough made in the discovery of BDPC (and it's homologues) is the need for a para substitution of the A-ring. Why para methyl and para bromo are the only examples with potent agonist activity was a mystery even to the inventor. The phenolic homologues of BDPC are, likewise, antagonists. But Chinese researchers showed that substitution of the 2-phenylethyl moiety with a 2-(2-thienyl)ethyl (C-8813) increased activity by the same factor as replacing the same moiety in the fentanyl scaffold.
I will conclude by noting that the discoverer of BDPC was able to construct a Drieding model and show that in it's active conformation, it perfectly overlayed the active conformation of fentanyl.
Note that the two aromatic rings (RAs), basic nitrogen (PIF) and oxygen (ELA). To quote the paper '...the molecues can be arranged as to give point for point coincidence for all of the salient features.'
While it's exteremely difficult to predict the QSAR of a novel compound, I am able to go two steps beyond the original paper by stating that the (R) enantiomer is the active and that the dimethyl homologue is an order of magnitude more potent than the monomethyl amine. The fact that researcher did NOT produce this seemily obvious homoogue can be explained by the reluctance of researchers to explicitly state that they have discovered a new class of potent MOR agonist.
Bioorganic & Medicinal Chemistry Letters Volume 10, Issue 6, 20 March 2000, Pages 523-526
Design, synthesis and biological evaluation of 3-amino-3-phenylpropionamide derivatives as novel μ opioid receptor ligands
Note that my research was based on compound 4a. Resolution of the enantiomers proved that it was the (R) enantiomer responsible for ALL the MOR activity and that N-methylation (modified Eschweiler–Clarke reaction) increased analgesic activity by an order of magnitue. I draw your attention to norbromidol (N-desmethyl BDPC) which is known to be an order of magnitude less potent than the parent drug.
Financial limitations prevented the Ki, or EC50 from being established but from a purely practical perspective, a simple in vivo model provided far more useful information i.e. the ED50 was measured. The ONLY thing were were unable to test was non-phenolic ring-substitutions. But if anyone cares to model the named compound with BDPC they will appreciate that both aromatic rings, the basic amine and the oxygen lone-pairs perfectly overlay those of BDPC. It would be nice if someone with the appropriate software could confirm that an appropriate para substitution would alter the activity in the same maner as the BDPC class.
postimg.cc
The above image includes several benzylamine class opioids. The relative spatial position of the aromatic(s), basic amine and oxygen function remains constant among them. The doxicopamine analogue is interesting because it's ED50 is given as 2.4mg/kg compared to 1.7mg/kg for morphine. Doxicopamine itself is considerable less potent and behaves as a mixed agonist/antagonist much like ciramadol. The meta pyridyl moiety of doxicopamine acting as a bioisostere of a meta hydroxy.
So we have at least a little more QSAR data.
Original paper: 'Analgetics. II. Relationship between structure and activity of some beta-amino ketones'
Paper in which para halo derivatives are tested: 'β-Amino Ketones. Synthesis and Some Biological Activities in mice of 3,3-Dialkyl-1,2,3,4-tetrahydro-4-quinolinones and Related Mannich Bases'
H - 16mg/Kg
F - 45mg/kg
Cl - 85 mg/kg
Like all good research, a negative result is still a valid and useful result.
What REALLY astounds me is that while the original paper does include some ring-substituted examples, it only covers ortho hydroxy and para methoxy examples. The meta hydroxy is not explored.
A further search revealed a rigid analogue which WAS an opioid AGONIST (and important detail as affinity ≠ effacacy) in the papers:
Opioid agonist and antagonist effects of configurational stereoisomers of 3-(dimethylamino)-2,2-dimethyl-7-hydroxy-1-tetralol
Opioid receptor effects of two 3-amino-2,2-dimethyltetralin analogs in guinea pig ileum longitudinal muscle
Opioid receptor effects of two aminotetralin derivatives using the electrically driven mouse vas deferens
But I was unable to locate ANY of the above papers (anyone?). The tetralin being phenolic and chiral revealed what is quite common. One enantiomer being an agonist, the other an antagonist.
I think most people have missed the fact that the simple, weak opioid discovered in the 1960s is closely related to the much more potent (3R)-2,2-dimethyl-3-(dimethylamino)-3-phenyl-N-(2-phenylethyl)propanamide class which itself overlays BDPC and ciramadol. In that case the phenolic derivatives are far more potent BUT the raecemates at least are antagonists. The KEY breaktrhough made in the discovery of BDPC (and it's homologues) is the need for a para substitution of the A-ring. Why para methyl and para bromo are the only examples with potent agonist activity was a mystery even to the inventor. The phenolic homologues of BDPC are, likewise, antagonists. But Chinese researchers showed that substitution of the 2-phenylethyl moiety with a 2-(2-thienyl)ethyl (C-8813) increased activity by the same factor as replacing the same moiety in the fentanyl scaffold.
I will conclude by noting that the discoverer of BDPC was able to construct a Drieding model and show that in it's active conformation, it perfectly overlayed the active conformation of fentanyl.
Note that the two aromatic rings (RAs), basic nitrogen (PIF) and oxygen (ELA). To quote the paper '...the molecues can be arranged as to give point for point coincidence for all of the salient features.'
While it's exteremely difficult to predict the QSAR of a novel compound, I am able to go two steps beyond the original paper by stating that the (R) enantiomer is the active and that the dimethyl homologue is an order of magnitude more potent than the monomethyl amine. The fact that researcher did NOT produce this seemily obvious homoogue can be explained by the reluctance of researchers to explicitly state that they have discovered a new class of potent MOR agonist.
Bioorganic & Medicinal Chemistry Letters Volume 10, Issue 6, 20 March 2000, Pages 523-526
Design, synthesis and biological evaluation of 3-amino-3-phenylpropionamide derivatives as novel μ opioid receptor ligands
Note that my research was based on compound 4a. Resolution of the enantiomers proved that it was the (R) enantiomer responsible for ALL the MOR activity and that N-methylation (modified Eschweiler–Clarke reaction) increased analgesic activity by an order of magnitue. I draw your attention to norbromidol (N-desmethyl BDPC) which is known to be an order of magnitude less potent than the parent drug.
Financial limitations prevented the Ki, or EC50 from being established but from a purely practical perspective, a simple in vivo model provided far more useful information i.e. the ED50 was measured. The ONLY thing were were unable to test was non-phenolic ring-substitutions. But if anyone cares to model the named compound with BDPC they will appreciate that both aromatic rings, the basic amine and the oxygen lone-pairs perfectly overlay those of BDPC. It would be nice if someone with the appropriate software could confirm that an appropriate para substitution would alter the activity in the same maner as the BDPC class.
1 — Postimages
The above image includes several benzylamine class opioids. The relative spatial position of the aromatic(s), basic amine and oxygen function remains constant among them. The doxicopamine analogue is interesting because it's ED50 is given as 2.4mg/kg compared to 1.7mg/kg for morphine. Doxicopamine itself is considerable less potent and behaves as a mixed agonist/antagonist much like ciramadol. The meta pyridyl moiety of doxicopamine acting as a bioisostere of a meta hydroxy.
