Intracerebroventricular administration of CYX-6, a potent μ-opioid receptor agonist, a δ- and κ-opioid receptor antagonist and a biased ligand at μ, δ &amp; κ-opioid receptors, evokes antinociception with minimal constipation and respiratory depression in rats in contrast to morphine

Imam, Mohammad Zafar; Kuo, Andy; Ghassabian, Sussan; Cai, Yunxin; Qin, Yajuan; Li, Tingyou; Smith, M. T.

doi:10.1016/j.ejphar.2020.172918

Cited by 13 publications

(31 citation statements)

References 52 publications

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“…The above observations demonstrated that combined chemical modifications of EMs would be helpful in improving their analgesic profiles with reduced unwanted opioid-like side effects. It was recently reported that the EM-2 derivative CYX-6 evoked potent antinociception with minimal constipation and respiratory depression . Novel macrocyclic tetrapeptide cyclo[Pro-Sar-Phe- d -Phe], a mixed opioid receptor agonist-antagonist, shows great promise for both the treatment of pain with reduced side effects and substance abuse and preventing both drug- and stress-induced relapse in morphine-abstinent subjects. , Zadina el al .…”

Section: Discussionmentioning

confidence: 99%

Novel Cyclic Endomorphin Analogues with Multiple Modifications and Oligoarginine Vector Exhibit Potent Antinociception with Reduced Opioid-like Side Effects

Zhang

Wang

et al. 2021

J. Med. Chem.

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Endomorphins (EMs) are potent pharmaceuticals for the treatment of pain. Herein, we investigated several novel EM analogues with multiple modifications and oligoarginine conjugation. Our results showed that analogues 1–6 behaved as potent μ-opioid agonists and enhanced stability and lipophilicity. Analogues 5 and 6 administered centrally and peripherally induced significant and prolonged antinociceptive effects in acute pain. Both analogues also produced long-acting antiallodynic effects against neuropathic and inflammatory pain. Furthermore, they showed a reduced acute antinociceptive tolerance. Analogue 6 decreased the extent of chronic antinociceptive tolerance, and analogue 5 exhibited no tolerance at the supraspinal level. Particularly, they displayed nontolerance-forming antinociception at the peripheral level. In addition, analogues 5 and 6 exhibited reduced or no opioid-like side effects on gastrointestinal transit, conditioned place preference (CPP), and motor impairment. The present investigation established that multiple modifications and oligoarginine-vector conjugation of EMs would be helpful in developing novel analgesics with fewer side effects.

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Section: Discussionmentioning

confidence: 99%

Novel Cyclic Endomorphin Analogues with Multiple Modifications and Oligoarginine Vector Exhibit Potent Antinociception with Reduced Opioid-like Side Effects

Zhang

Wang

et al. 2021

J. Med. Chem.

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“…In other work, CYX-6 (Dmt-Pro-Tmp-Tmp-NH 2 ) ( 98 ) (Figure ) produced an interesting profile as a potent MOP agonist with DOP and KOP antagonist activities in the cAMP assay . In a rat model of nociceptive pain, icv CYX-6 ( 98 ) evoked potent dose-dependent naloxone-sensitive antinociception, confirming that antinociception was opioid-receptor-mediated . No gastrointestinal adverse effects were observed with icv CYX-6 ( 98 ) as measured by the inhibition of gastrointestinal transit or castor oil induced-diarrahea (constipation assays), in contrast to icv morphine ( 1 ) (Figure ).…”

Section: Opioid Peptides As Drug Leadsmentioning

confidence: 91%

Analgesic Opioid Ligand Discovery Based on Nonmorphinan Scaffolds Derived from Natural Sources

et al. 2022

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Strong opioid analgesics, including morphine, are the mainstays for treating moderate to severe acute pain and alleviating chronic cancer pain. However, opioid-related adverse effects, including nausea or vomiting, sedation, respiratory depression, constipation, pruritus (itch), analgesic tolerance, and addiction and abuse liability, are problematic. In addition, the use of opioids to relieve chronic noncancer pain is controversial due to the “opioid crisis” characterized by opioid misuse or abuse and escalating unintentional death rates due to respiratory depression. Hence, considerable research internationally has been aimed at the “Holy Grail” of the opioid analgesic field, namely the discovery of novel and safer opioid analgesics with improved opioid-related adverse effects. In this Perspective, medicinal chemistry strategies are addressed, where structurally diverse nonmorphinan-based opioid ligands derived from natural sources were deployed as lead molecules. The current state of play, clinical or experimental status, and novel opioid ligand discovery approaches are elaborated in the context of retaining analgesia with improved safety and reduced adverse effects, especially addiction liability.

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“…The desired product was obtained as colorless oil (640 mg, 91% yield). 1 4-(7-Cyano-3,4-dihydroisoquinolin-2(1H)-yl)-N,N-dimethyl-2,2diphenylbutanamide (24). The reaction was performed following the same procedure described for 23, starting from 1,2,3,4-tetrahydroisoquinoline-7-carbonitrile (100 mg, 0.63 mmol).…”

Section: ■ Experimental Methodsmentioning

confidence: 99%

“…Design, synthesis, and pharmacological characterization of signaling-pathway-biased agonists targeting the MORs allowed the identification of highly selective G-protein-biased agonists, with limited activation of β-arrestin pathways, highlighting different physiological effects mediated by each independent pathway. , It has been suggested that the MOR G-protein pathway seems to be the predominant mediator of the analgesic effects of MOR agonists; meanwhile, it has been posited that the simultaneous hindering of β-arrestin recruitment might reduce the respiratory depression and other side effects, such as constipation, associated with opioid-like drugs. − However, this has been a topic of intensive investigation, and recently, it has been reported that classical MOR agonists, such as morphine and fentanyl , induce dose-dependent respiratory depression and constipation in β-arrestin-2 knock-out mice, similar to what is observed in wild-type mice. − Subsequent pharmacological evaluation has also shown that MOR G-protein-biased agonists still have abuse potential. ,− It is still unclear whether the optimal outcome and pharmacotherapeutic potential of MOR agonists can be gained through selective activation of a particular downstream signaling pathway (functional selectivity) or whether an optimal level partial agonism at multiple pathways may instead provide a route for the development of safer opioids. , Independent of the signaling pathways and cellular mechanisms associated with respiratory depression and constipation, abuse liability remains as a serious concern that must be addressed with different drug design approaches.…”

Section: Introductionmentioning

confidence: 99%

Novel Dual-Target μ-Opioid Receptor and Dopamine D₃ Receptor Ligands as Potential Nonaddictive Pharmacotherapeutics for Pain Management

et al. 2021

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The need for safer pain-management therapies with decreased abuse liability inspired a novel drug design that retains μ-opioid receptor (MOR)-mediated analgesia, while minimizing addictive liability. We recently demonstrated that targeting the dopamine D3 receptor (D3R) with highly selective antagonists/partial agonists can reduce opioid self-administration and reinstatement to drug seeking in rodent models without diminishing antinociceptive effects. The identification of the D3R as a target for the treatment of opioid use disorders prompted the idea of generating a class of ligands presenting bitopic or bivalent structures, allowing the dual-target binding of the MOR and D3R. Structure–activity relationship studies using computationally aided drug design and in vitro binding assays led to the identification of potent dual-target leads (23, 28, and 40), based on different structural templates and scaffolds, with moderate (sub-micromolar) to high (low nanomolar/sub-nanomolar) binding affinities. Bioluminescence resonance energy transfer-based functional studies revealed MOR agonist–D3R antagonist/partial agonist efficacies that suggest potential for maintaining analgesia with reduced opioid-abuse liability.

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Intracerebroventricular administration of CYX-6, a potent μ-opioid receptor agonist, a δ- and κ-opioid receptor antagonist and a biased ligand at μ, δ & κ-opioid receptors, evokes antinociception with minimal constipation and respiratory depression in rats in contrast to morphine

Cited by 13 publications

References 52 publications

Novel Cyclic Endomorphin Analogues with Multiple Modifications and Oligoarginine Vector Exhibit Potent Antinociception with Reduced Opioid-like Side Effects

Novel Cyclic Endomorphin Analogues with Multiple Modifications and Oligoarginine Vector Exhibit Potent Antinociception with Reduced Opioid-like Side Effects

Analgesic Opioid Ligand Discovery Based on Nonmorphinan Scaffolds Derived from Natural Sources

Novel Dual-Target μ-Opioid Receptor and Dopamine D₃ Receptor Ligands as Potential Nonaddictive Pharmacotherapeutics for Pain Management

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Intracerebroventricular administration of CYX-6, a potent μ-opioid receptor agonist, a δ- and κ-opioid receptor antagonist and a biased ligand at μ, δ & κ-opioid receptors, evokes antinociception with minimal constipation and respiratory depression in rats in contrast to morphine

Cited by 13 publications

References 52 publications

Novel Cyclic Endomorphin Analogues with Multiple Modifications and Oligoarginine Vector Exhibit Potent Antinociception with Reduced Opioid-like Side Effects

Novel Cyclic Endomorphin Analogues with Multiple Modifications and Oligoarginine Vector Exhibit Potent Antinociception with Reduced Opioid-like Side Effects

Analgesic Opioid Ligand Discovery Based on Nonmorphinan Scaffolds Derived from Natural Sources

Novel Dual-Target μ-Opioid Receptor and Dopamine D3 Receptor Ligands as Potential Nonaddictive Pharmacotherapeutics for Pain Management

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Product

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Novel Dual-Target μ-Opioid Receptor and Dopamine D₃ Receptor Ligands as Potential Nonaddictive Pharmacotherapeutics for Pain Management