Chemical compound
Pharmaceutical compound
Darigabat (developmental code names CVL-865 , PF-06372865 , PF-6372865 ) is a GABAergic medication which is under development for the treatment of photosensitive epilepsy , focal onset seizures , panic disorder , and other anxiety disorders .[ 2] [ 3] It was also under development for the treatment of generalized anxiety disorder and chronic lower back pain , but development for these indications was discontinued.[ 2] [ 3] [ 4] It is taken via oral administration .[ 2]
Darigabat acts as a GABAA receptor positive allosteric modulator [ 2] [ 3] [ 5] It is specifically a positive allosteric modulator that selectively targets α2 , α3 , and α5 subunit -containing GABAA receptors , with minimal functional activity at α1 subunit -containing GABAA receptors.[ 3] [ 5] A dose of darigabat that achieved more than 80% receptor occupancy showed no somnolence with dose titration , whereas benzodiazepines , which are non-selective GABAA receptor positive allosteric modulators, achieve only 10 to 15% receptor occupancy whilst producing significant or severe somnolence.[ 3] [ 5] It is theorized that α1 subunit-containing GABAA receptors preferentially mediate sedation , amnesia , and ataxia , whereas α2 and α3 subunit-containing GABAA receptors mediate anxiolysis .[ 3] [ 5] However, this model has also been questioned.[ 4] α1 subunit-containing GABAA receptors are said to be completely unaffected by darigabat.[ 6] The elimination half-life of darigabat is 11 hours and it is metabolized mainly by CYP3A4 .[ 1]
In clinical trials conducted thus far, side effects of darigabat have included dizziness , fatigue , headache , mild-to-moderate somnolence , bradyphrenia (slowness of thought), modest memory impairment , mild cognitive impairment , balance impairment , and feeling abnormal.[ 3] [ 6] It has been described as well-tolerated .[ 3] [ 4]
Darigabat was originated by Pfizer and is under development by Cerevel Therapeutics and Pfizer .[ 2] As of January 2023, it is in phase 2 clinical trials for epilepsy and seizures, phase 1 trials for panic disorder, and preclinical development for anxiety disorders.[ 2] [ 3] Development for back pain was discontinued due to lack of effectiveness in a phase 2 trial, while development for generalized anxiety disorder was discontinued due to business reasons as well as lack of effectiveness in a phase 2 trial.[ 3] [ 4] [ 2]
See also
References
^ a b c Elkommos S, Mula M (December 2022). "Current and future pharmacotherapy options for drug-resistant epilepsy". Expert Opin Pharmacother . 23 (18): 2023– 2034. doi :10.1080/14656566.2022.2128670 . PMID 36154780 . S2CID 252542159 .
^ a b c d e f g "Darigabat - Cerevel Therapeutics - AdisInsight" .
^ a b c d e f g h i j Cerne R, Lippa A, Poe MM, Smith JL, Jin X, Ping X, Golani LK, Cook JM, Witkin JM (June 2022). "GABAkines - Advances in the discovery, development, and commercialization of positive allosteric modulators of GABAA receptors" . Pharmacol Ther . 234 : 108035. doi :10.1016/j.pharmthera.2021.108035 . PMC 9787737 . PMID 34793859 .
^ a b c d Witkin JM, Lippa A, Smith JL, Jin X, Ping X, Biggerstaff A, Kivell BM, Knutson DE, Sharmin D, Pandey KP, Mian MY, Cook JM, Cerne R (February 2022). "The imidazodiazepine, KRM-II-81: An example of a newly emerging generation of GABAkines for neurological and psychiatric disorders". Pharmacol Biochem Behav . 213 : 173321. doi :10.1016/j.pbb.2021.173321 . PMID 35041859 . S2CID 245963990 .
^ a b c d Quagliato LA, Carta MG, Nardi AE (2022). "Panic Disorder Seeks More Specific Drugs for Treatment: Might the Amygdala Be the Best Target?". J Clin Psychopharmacol . 42 (5): 427– 428. doi :10.1097/JCP.0000000000001591 . PMID 36099401 . S2CID 252219658 .
^ a b Janković SM, Dješević M, Janković SV (2021). "Experimental GABA A Receptor Agonists and Allosteric Modulators for the Treatment of Focal Epilepsy" . J Exp Pharmacol . 13 : 235– 244. doi :10.2147/JEP.S242964 . PMC 7954424 . PMID 33727865 .
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