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Your search keyword '"Portoghese, Philip S."' showing total 15 results

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15 results on '"Portoghese, Philip S."'

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1. A bivalent compound targeting CCR5 and the mu opioid receptor treats inflammatory arthritis pain in mice without inducing pharmacologic tolerance.

2. Bivalent ligand MCC22 potently attenuates nociception in a murine model of sickle cell disease.

3. Bivalent ligand that activates mu opioid receptor and antagonizes mGluR5 receptor reduces neuropathic pain in mice.

4. Inhibition of Inflammatory and Neuropathic Pain by Targeting a Mu Opioid Receptor/Chemokine Receptor5 Heteromer (MOR-CCR5).

5. Targeting putative mu opioid/metabotropic glutamate receptor-5 heteromers produces potent antinociception in a chronic murine bone cancer model.

6. Putative kappa opioid heteromers as targets for developing analgesics free of adverse effects.

7. Clinically employed opioid analgesics produce antinociception via μ-δ opioid receptor heteromers in Rhesus monkeys.

8. Opioid activity of spinally selective analogues of N-naphthoyl-β-naltrexamine in HEK-293 cells and mice.

9. N-naphthoyl-beta-naltrexamine (NNTA), a highly selective and potent activator of μ/kappa-opioid heteromers.

10. Naloxone acts as a potent analgesic in transgenic mouse models of sickle cell anemia.

11. Opioid-induced tolerance and dependence in mice is modulated by the distance between pharmacophores in a bivalent ligand series.

12. A heterodimer-selective agonist shows in vivo relevance of G protein-coupled receptor dimers.

13. N-naphthoyl-β-naltrexamine (NNTA), a highly selective and potent activator of μ/κ-opioid heteromers.

14. The bivalent ligand, MMG22, reduces neuropathic pain after nerve injury without the side effects of traditional opioids.

15. MDAN-21: A Bivalent Opioid Ligand Containing mu-Agonist and Delta-Antagonist Pharmacophores and Its Effects in Rhesus Monkeys.

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