Synthesis of Carfentanil Amide Opioids Using the Ugi Multicomponent Reaction

Váradi, András; Palmer, Travis C.; Haselton, Nathan; Afonin, D.G.; Subrath, Joan; Rouzic, Valerie Le; Hunkele, Amanda; Pasternak, Gavril W.; Marrone, Gina F.; Borics, Attila; Majumdar, Susruta

doi:10.1021/acschemneuro.5b00137

Cited by 41 publications

(49 citation statements)

References 38 publications

(44 reference statements)

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“…7–9,80 Binding was performed at 25 °C for 90 min. Binding in MOR-1/CHO was carried out in 50 mM potassium phosphate buffer with 5 mM MgSO 4 and 20 μ g/mL protein, while binding in KOR-1/CHO and DOR-1/CHO was carried out in 50 mM potassium phosphate pH = 7.0 buffer and 40 μ g/mL protein.…”

Section: Methodsmentioning

confidence: 99%

“…8,9 The intensity was set to achieve a baseline between 2 and 3 s. Baseline latencies were determined before experimental treatments for all mice. Tail flick antinociception was assessed quantally as a doubling or greater of the baseline latency, with a maximal 10 s latency to minimize damage to the tail.…”

Section: Methodsmentioning

confidence: 99%

“…Many approaches have been taken over the years, starting with the development of partial agonists or mixed agonist/antagonists. 5–9 A more recent approach takes advantage of biased agonism, in which distinct downstream signaling pathways are activated by different agonists working through the same receptor. 10,11 It has been proposed that ligands biased against recruiting β -arrestin-2, or showing preference for activating specific G-protein-mediated signal transduction pathways, will demonstrate diminished side effects.…”

Section: Introductionmentioning

confidence: 99%

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Mitragynine/Corynantheidine Pseudoindoxyls As Opioid Analgesics with Mu Agonism and Delta Antagonism, Which Do Not Recruit β-Arrestin-2

et al. 2016

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Natural products found in Mitragyna speciosa, commonly known as kratom, represent diverse scaffolds (indole, indolenine, and spiro pseudoindoxyl) with opioid activity, providing opportunities to better understand opioid pharmacology. Herein, we report the pharmacology and SAR studies both in vitro and in vivo of mitragynine pseudoindoxyl (3), an oxidative rearrangement product of the corynanthe alkaloid mitragynine. 3 and its corresponding corynantheidine analogs show promise as potent analgesics with a mechanism of action that includes mu opioid receptor agonism/delta opioid receptor antagonism. In vitro, 3 and its analogs were potent agonists in [35S]GTPγS assays at the mu opioid receptor but failed to recruit β-arrestin-2, which is associated with opioid side effects. Additionally, 3 developed analgesic tolerance more slowly than morphine, showed limited physical dependence, respiratory depression, constipation, and displayed no reward or aversion in CPP/CPA assays, suggesting that analogs might represent a promising new generation of novel pain relievers.

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Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Mitragynine/Corynantheidine Pseudoindoxyls As Opioid Analgesics with Mu Agonism and Delta Antagonism, Which Do Not Recruit β-Arrestin-2

et al. 2016

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“…Interestingly, two analogs in the same series with a t-butyl amide group ( N -( tert -butyl)-1-phenethyl-4-( N -phenylpropionamido)piperidine-4-carboxamide, MP105 ) and cyclopropyl amide group ( N -cyclopropyl-1-phenethyl-4-( N -phenylpropionamido)piperidine-4-carboxamide, MP103 ) instead of cycloheptyl amide moiety showed higher efficacy in the β-arrestin 2 assay compared to MP102, again suggesting that small changes in structure of the analog lead to differential signaling ( Table 1 ). A lead compound in this series MP102 [ 25 , 52 ] exhibited moderately potent analgesia with significantly reduced respiratory depression, constipation, and physical dependence while showing analgesic tolerance and reward behavior. The role of DOR agonism in the actions of MP102 may play a key role in vivo and needs to be investigated with future analog design.…”

Section: Mor Biased Agonismmentioning

confidence: 99%

Biased Opioid Ligands

2020

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Achieving effective pain management is one of the major challenges associated with modern day medicine. Opioids, such as morphine, have been the reference treatment for moderate to severe acute pain not excluding chronic pain modalities. Opioids act through the opioid receptors, the family of G-protein coupled receptors (GPCRs) that mediate pain relief through both the central and peripheral nervous systems. Four types of opioid receptors have been described, including the μ-opioid receptor (MOR), κ-opioid receptor (KOR), δ-opioid receptor (DOR), and the nociceptin opioid peptide receptor (NOP receptor). Despite the proven success of opioids in treating pain, there are still some inherent limitations. All clinically approved MOR analgesics are associated with adverse effects, which include tolerance, dependence, addiction, constipation, and respiratory depression. On the other hand, KOR selective analgesics have found limited clinical utility because they cause sedation, anxiety, dysphoria, and hallucinations. DOR agonists have also been investigated but they have a tendency to cause convulsions. Ligands targeting NOP receptor have been reported in the preclinical literature to be useful as spinal analgesics and as entities against substance abuse disorders while mixed MOR/NOP receptor agonists are useful as analgesics. Ultimately, the goal of opioid-related drug development has always been to design and synthesize derivatives that are equally or more potent than morphine but most importantly are devoid of the dangerous residual side effects and abuse potential. One proposed strategy is to take advantage of biased agonism, in which distinct downstream pathways can be activated by different molecules working through the exact same receptor. It has been proposed that ligands not recruiting β-arrestin 2 or showing a preference for activating a specific G-protein mediated signal transduction pathway will function as safer analgesic across all opioid subtypes. This review will focus on the design and the pharmacological outcomes of biased ligands at the opioid receptors, aiming at achieving functional selectivity.

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“…Over hundred million people in the United States suffer from chronic and neuropathic pain. 1 The morphine structure was discovered in 1803 by the German pharmacist Serturner, but only in the last 40 years researchers have made important progress in opioid drug discovery 2–13 based on the natural endogenous opioid ligands. Including the molecularly cloned three opioid receptors (μ, δ and κ) and have a better understanding of mechanism of action, and the recent crystallographic analysis of μ and other opioid receptors.…”

Section: Introductionmentioning

confidence: 99%

Design synthesis and structure–activity relationship of 5-substituted (tetrahydronaphthalen-2yl)methyl with N-phenyl-N-(piperidin-2-yl)propionamide derivatives as opioid ligands

Srinivas

Rankin

Davis

et al. 2016

Bioorganic & Medicinal Chemistry

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Here, we report the design, synthesis and structure activity relationship of novel small molecule opioid ligands based on 5-amino substituted (tetrahydronaphthalen-2-yl)methyl moiety with N-phenyl-N-(piperidin-2-yl)propionamide derivatives. We synthesized various molecules including amino, amide and hydroxy substitution on the 5th position of the (tetrahydronaphthalen-2-yl)methyl moiety. In our further designs we replaced the (tetrahydronaphthalen-2-yl)methyl moiety with benzyl and phenethyl moiety. These N-phenyl-N-(piperidin-2-yl)propionamide analogues showed moderate to good binding affinities (850–4 nM) and were selective towards the μ opioid receptor over the δ opioid receptors. From the structure activity relationship studies, we found that a hydroxyl substitution at the 5th position of (tetrahydronapthalen-2yl)methyl group, ligands 19 and 20, showed excellent binding affinities 4 and 5 nM, respectively, and 1000 fold selectivity towards the μ opioid relative to the delta opioid receptor. The ligand 19 showed potent agonist activities 75 ± 21 nM, and 190 ± 42 nM in the GPI and MVD assays. Surprisingly the fluoro analogue 20 showed good agonist activities in MVD assays 170 ± 42 nM, in contrast to its binding affinity results.

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Synthesis of Carfentanil Amide Opioids Using the Ugi Multicomponent Reaction

Cited by 41 publications

References 38 publications

Mitragynine/Corynantheidine Pseudoindoxyls As Opioid Analgesics with Mu Agonism and Delta Antagonism, Which Do Not Recruit β-Arrestin-2

Mitragynine/Corynantheidine Pseudoindoxyls As Opioid Analgesics with Mu Agonism and Delta Antagonism, Which Do Not Recruit β-Arrestin-2

Biased Opioid Ligands

Design synthesis and structure–activity relationship of 5-substituted (tetrahydronaphthalen-2yl)methyl with N-phenyl-N-(piperidin-2-yl)propionamide derivatives as opioid ligands

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