Discovery of the First Vitamin K Analogue as a Potential Treatment of Pharmacoresistant Seizures.
Xiaoyang LiRichard A HimesLyndsey C ProsserCharleston F ChristieEmma WattSharon F EdwardsCameron S MetcalfPeter J WestKaren S WilcoxSherine S L ChanC James ChouPublished in: Journal of medicinal chemistry (2020)
Despite the availability of more than 25 antiseizure drugs on the market, approximately 30% of patients with epilepsy still suffer from seizures. Thus, the epilepsy therapy market has a great need for a breakthrough drug that will aid pharmacoresistant patients. In our previous study, we discovered a vitamin K analogue, 2h, which displayed modest antiseizure activity in zebrafish and mouse seizure models. However, there are limitations to this compound due to its pharmacokinetic profile. In this study, we develop a new series of vitamin K analogues by modifying the structure of 2h. Among these, compound 3d shows full protection in a rodent pharmacoresistant seizure model with limited rotarod motor toxicity and favorable pharmacokinetic properties. Furthermore, the brain/plasma concentration ratio of 3d indicates its excellent permeability into the brain. The resulting data shows that 3d can be further developed as a potential antiseizure drug in the clinic.
Keyphrases
- temporal lobe epilepsy
- newly diagnosed
- primary care
- health insurance
- oxidative stress
- resting state
- stem cells
- emergency department
- risk assessment
- multiple sclerosis
- prognostic factors
- endothelial cells
- cerebral ischemia
- combination therapy
- blood brain barrier
- patient reported outcomes
- artificial intelligence
- human health
- adverse drug
- molecular docking
- cell therapy
- structure activity relationship