A Comparison of the 2/3/5 Selective Positive Allosteric Modulators L-838,417 and TPA023 in Preclinical Models of Inflammatory and Neuropathic Pain

Author:

Nickolls Sarah1,Mace Hannah1,Fish Rebecca1,Edye Michelle1,Gurrell Rachel1ORCID,Ivarsson Magnus1,Pitcher Tom1,Tanimoto-Mori Sachi1,Richardson Denise1,Sweatman Catherine1,Nicholson Janet1,Ward Cameron1,Jinks John1,Bell Christine1,Young Kimberly1,Rees Huw1,Moss Andrew1,Kinloch Ross1,McMurray Gordon1

Affiliation:

1. Discovery Biology, Pfizer Inc., Ramsgate Road, Sandwich, Kent CT13 9NJ, UK

Abstract

receptors containingα2/3 subunits are current targets in the battle to develop new pain medications, as they are expressed in the spinal cord where increasing inhibitory drive should result in analgesia. However, this approach is prone to a range of side effects including sedation, cognitive impairment, and abuse as a consequence of the widespread influence of GABA. The ability to make subtype selective low-efficacy benzodiazepine compounds, which potentiate the action of GABA at specificαsubunits, has the potential to reduce this side effect profile. In this study, we have investigated the effects of the medium-efficacy positive allosteric modulator (PAM) L-838,417 and the low-efficacy PAM TPA023 in a number of preclinical inflammatory and neuropathic pain models. We conclude that either the higher level of efficacy atα2/3 or efficacy atα5 is required for compounds to have a significant analgesic effect in a range of models, and, therefore, although the side-effect profile of compounds can be reduced compared to typical benzodiazepines, it is unlikely that it can be completely eliminated.

Publisher

Hindawi Limited

Subject

Pharmacology (medical),General Pharmacology, Toxicology and Pharmaceutics,Molecular Medicine

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