Your search keyword '"Sassano MF"' showing total 2 results

1. Structure-based discovery of opioid analgesics with reduced side effects.

Author

Manglik A, Lin H, Aryal DK, McCorvy JD, Dengler D, Corder G, Levit A, Kling RC, Bernat V, Hübner H, Huang XP, Sassano MF, Giguère PM, Löber S, Da Duan, Scherrer G, Kobilka BK, Gmeiner P, Roth BL, and Shoichet BK

Subjects

Analgesia methods, Analgesics, Opioid pharmacology, Animals, GTP-Binding Protein alpha Subunits, Gi-Go metabolism, HEK293 Cells, Humans, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Molecular Docking Simulation, Pain drug therapy, Receptors, Opioid, mu deficiency, Receptors, Opioid, mu genetics, Receptors, Opioid, mu metabolism, Spiro Compounds pharmacology, Structure-Activity Relationship, Thiophenes adverse effects, Urea adverse effects, Urea chemistry, Urea pharmacology, Analgesics, Opioid adverse effects, Analgesics, Opioid chemistry, Drug Discovery, Receptors, Opioid, mu agonists, Thiophenes chemistry, Thiophenes pharmacology, Urea analogs & derivatives

Abstract

Morphine is an alkaloid from the opium poppy used to treat pain. The potentially lethal side effects of morphine and related opioids-which include fatal respiratory depression-are thought to be mediated by μ-opioid-receptor (μOR) signalling through the β-arrestin pathway or by actions at other receptors. Conversely, G-protein μOR signalling is thought to confer analgesia. Here we computationally dock over 3 million molecules against the μOR structure and identify new scaffolds unrelated to known opioids. Structure-based optimization yields PZM21-a potent G i activator with exceptional selectivity for μOR and minimal β-arrestin-2 recruitment. Unlike morphine, PZM21 is more efficacious for the affective component of analgesia versus the reflexive component and is devoid of both respiratory depression and morphine-like reinforcing activity in mice at equi-analgesic doses. PZM21 thus serves as both a probe to disentangle μOR signalling and a therapeutic lead that is devoid of many of the side effects of current opioids., Competing Interests: The authors declare competing financial interests: details are available in the online version of the paper. Readers are welcome to comment on the online version of the paper.

Published

2016

2. Automated design of ligands to polypharmacological profiles.

Author

Besnard J, Ruda GF, Setola V, Abecassis K, Rodriguiz RM, Huang XP, Norval S, Sassano MF, Shin AI, Webster LA, Simeons FR, Stojanovski L, Prat A, Seidah NG, Constam DB, Bickerton GR, Read KD, Wetsel WC, Gilbert IH, Roth BL, and Hopkins AL

Subjects

Animals, Automation, Drug Delivery Systems, Female, Male, Mice, Mice, Inbred C57BL, Models, Theoretical, Pharmacological Phenomena, Reproducibility of Results, Drug Design, Ligands

Abstract

The clinical efficacy and safety of a drug is determined by its activity profile across many proteins in the proteome. However, designing drugs with a specific multi-target profile is both complex and difficult. Therefore methods to design drugs rationally a priori against profiles of several proteins would have immense value in drug discovery. Here we describe a new approach for the automated design of ligands against profiles of multiple drug targets. The method is demonstrated by the evolution of an approved acetylcholinesterase inhibitor drug into brain-penetrable ligands with either specific polypharmacology or exquisite selectivity profiles for G-protein-coupled receptors. Overall, 800 ligand-target predictions of prospectively designed ligands were tested experimentally, of which 75% were confirmed to be correct. We also demonstrate target engagement in vivo. The approach can be a useful source of drug leads when multi-target profiles are required to achieve either selectivity over other drug targets or a desired polypharmacology.

Published

2012