Discovery and Profiling of New Multimodal Phenylglycinamide Derivatives As Potent Antiseizure and Antinociceptive Drug Candidates

Overview

Journal ACS Chem Neurosci

Publisher American Chemical Society

Specialty Neurology

Date 2024 Aug 21

PMID 39166702

Authors

Marcin Jakubiec

Michal Abram

Miroslaw Zagaja

Katarzyna Socala

Vanja Panic

Gniewomir Latacz

Szczepan Mogilski

Malgorzata Szafarz

Joanna Szala-Rycaj

Jerry Saunders

Peter J West

Dorota Nieoczym

Katarzyna Przejczowska-Pomierny

Bartlomiej Szulczyk

Anna Krupa

Elzbieta Wyska

Piotr Wlaz

Cameron S Metcalf

Karen Wilcox

Marta Andres-Mach

Rafal M Kaminski

Krzysztof Kaminski

Affiliations

Soon will be listed here.

Abstract

We developed a focused series of original phenyl-glycinamide derivatives which showed potent activity across mouse seizure models, namely, maximal electroshock (MES) and 6 Hz (using both 32 and 44 mA current intensities) seizure models. Following intraperitoneal (.) administration, compound , which was identified as a lead molecule, demonstrated potent protection against all seizure models with ED values of 73.9 mg/kg (MES test), 18.8 mg/kg (6 Hz, 32 mA test), and 26.5 mg/kg (6 Hz, 44 mA test). Furthermore, demonstrated efficacy in both the PTZ-induced kindling paradigm and the PTZ seizure threshold test. The expression of neurotrophic factors, such as mature brain-derived neurotrophic factor (mBDNF) and nerve growth factor (NGF), in the hippocampus and/or cortex of mice, and the levels of glutamate and GABA were normalized after PTZ-induced kindling by . Importantly, besides antiseizure activity, () demonstrated potent antinociceptive efficacy in formalin-induced pain, capsaicin-induced pain, as well as oxaliplatin- and streptozotocin-induced peripheral neuropathy in mice (.). No influence on muscular strength and body temperature in mice was observed. Pharmacokinetic studies and ADME-Tox data (, high metabolic stability in human liver microsomes, a weak influence on CYPs, no hepatotoxicity, satisfactory passive transport, ) proved favorable drug-like properties of (). Thermal stability of ()- shown in thermogravimetry and differential scanning calorimetry gives the opportunity to develop innovative oral solid dosage forms loaded with this compound. The binding and functional assays indicated its multimodal mechanism of action. (), beyond TRPV1 antagonism, inhibited calcium and sodium currents at a concentration of 10 μM. Therefore, the data obtained in the current studies justify a more detailed preclinical development of () for epilepsy and pain indications.

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