Development of Inhaled GABA_A Receptor Modulators to Improve Airway Function in Bronchoconstrictive Disorders

Abstract: We report the modification of MIDD0301, an imidazodiazepine GABA A receptor (GABA A R) ligand, using two alkyl substituents. We developed PI310 with a 6-(4-phenylbutoxy)hexyl chain as used in the long-acting β2-agonist salmeterol and PI320 with a poly(ethylene glycol) chain as used to improve the brain:plasma ratio of naloxegol, a naloxone analogue. Both imidazodiazepines showed affinity toward the GABA A R binding site of clonazepam, with IC 50 values of 576 and 242 nM, respectively. Molecular docking analysi… Show more

“…Furthermore, hydrogen bond interactions between the carboxylate and Ser206 and Ser205 and the imine function were identified. We reported molecular docking poses for MIDD0301 bearing a (R) or (S) methyl substituent instead of the cyclopropyl substituent and observed the almost same docking poses . The stereochemistry of the methyl substituent did not significantly influence GABA A R binding ( MIDD0301 (IC 50 = 26 nM) and MIDD0301S (IC 50 = 25 nM)).…”

“…We previously reported that MIDD0301 potently relaxes constricted airway smooth muscle ex vivo and reduces AHR in vivo. ,,, For the ex vivo experiment, guinea pig tracheal rings were suspended in an organ bath, constricted with substance-P, and treated with 5a–j followed by recording of muscle force (Figure ).…”

“…We reported molecular docking poses for MIDD0301 bearing a (R) or (S) methyl substituent instead of the cyclopropyl substituent and observed the almost same docking poses. 29 The stereochemistry of the methyl substituent did not significantly influence GABA A R binding (MIDD0301 (IC 50 = 26 nM) and MIDD0301S (IC 50 = 25 nM)). Based on this knowledge, we used molecular operating environment (MOE) software to compute binding scores of other synthesized GABA A R ligands.…”

Design, Synthesis, and Biological Evaluation of Novel Spiro Imidazobenzodiazepines to Identify Improved Inhaled Bronchodilators

“…Furthermore, hydrogen bond interactions between the carboxylate and Ser206 and Ser205 and the imine function were identified. We reported molecular docking poses for MIDD0301 bearing a (R) or (S) methyl substituent instead of the cyclopropyl substituent and observed the almost same docking poses . The stereochemistry of the methyl substituent did not significantly influence GABA A R binding ( MIDD0301 (IC 50 = 26 nM) and MIDD0301S (IC 50 = 25 nM)).…”

“…We previously reported that MIDD0301 potently relaxes constricted airway smooth muscle ex vivo and reduces AHR in vivo. ,,, For the ex vivo experiment, guinea pig tracheal rings were suspended in an organ bath, constricted with substance-P, and treated with 5a–j followed by recording of muscle force (Figure ).…”

“…We reported molecular docking poses for MIDD0301 bearing a (R) or (S) methyl substituent instead of the cyclopropyl substituent and observed the almost same docking poses. 29 The stereochemistry of the methyl substituent did not significantly influence GABA A R binding (MIDD0301 (IC 50 = 26 nM) and MIDD0301S (IC 50 = 25 nM)). Based on this knowledge, we used molecular operating environment (MOE) software to compute binding scores of other synthesized GABA A R ligands.…”

Design, Synthesis, and Biological Evaluation of Novel Spiro Imidazobenzodiazepines to Identify Improved Inhaled Bronchodilators

Experimental study and thermodynamic modeling of clonazepam solubility in supercritical carbon dioxide

Peripheral GABAA receptors - Physiological relevance and therapeutic implications