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The Structure-Activity Relatıonships of Familiar Antiepileptic Drugs and Na+ Channels

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dc.contributor.authorÇAKMAK, Esra Nur
dc.contributor.authorGÜR, Mahmut
dc.contributor.authorKIRAN, Bayram
dc.date.accessioned2026-01-04T16:59:44Z
dc.date.issued2022-06-30
dc.description.abstractThe aim of this study is to examine the effects of drug active compounds, which are widely used in the treatment of epilepsy, on voltage-gated Na+ channels are important channels that advance the action potential in the excitation direction by molecular docking method. These molecules have been selected considering the physiopathological effect mechanisms of epilepsy disease. When the action potential is stimulated, Na+ channels allow sodium ion entry into the cell and cause epilepsy seizures. For this reason, PDB ID: 4PA6 receptor, which acts as an antagonist according to its activity on the canal in the formation of epileptic seizures, was chosen for molecular docking study. As a result of molecular docking studies; Phenytoin gave the best binding affinity for 4PA6 with a value of -7.7 kcal/mol. Other results in descending order (as kcal/mol); Mesuximide (-7.5), Remasemide (-7.3), Tiagabine (-7.1), Ethotoin and Mephenytoin (-7.0), Primidon (-6.9), Topiramate (-6.6), Oxcarbazepine and Lamotrigin (-6.3), Felbamat (-6.0), Lokosamidine (-5.9), Zonisamide (-5.8), Levetiresetam and Gabapentin (-5.7), Ethosuximide (-5.6), Trimethadion (-5.1), Valproic Acid (-5.0), Vigabatrin (-4.0), determined as.
dc.description.urihttps://doi.org/10.17350/hjse19030000259
dc.description.urihttps://doaj.org/article/cb44608275584998b1e3cc19c59ce5d5
dc.description.urihttps://dergipark.org.tr/tr/pub/hjse/issue/70658/1047636
dc.identifier.doi10.17350/hjse19030000259
dc.identifier.eissn2148-4171
dc.identifier.endpage102
dc.identifier.openairedoi_dedup___::24a617a06d1b7f5bf8634748e6c9d0bf
dc.identifier.orcid0000-0003-4033-5190
dc.identifier.orcid0000-0001-9942-6324
dc.identifier.orcid0000-0001-9796-6028
dc.identifier.startpage89
dc.identifier.urihttps://hdl.handle.net/20.500.12597/39824
dc.identifier.volume9
dc.publisherHitit University
dc.relation.ispartofHittite Journal of Science and Engineering
dc.rightsOPEN
dc.subjectEngineering
dc.subjectmoleculer docking
dc.subjectAnticonvulsant
dc.subjectEpilepsy
dc.subjectMoleculer Docking
dc.subjectLigand
dc.subjectReceptor
dc.subjectreceptor
dc.subjectMühendislik
dc.subjectepilepsy
dc.subjectTA1-2040
dc.subjectanticonvulsant
dc.subjectligand
dc.subjectEngineering (General). Civil engineering (General)
dc.subject.sdg3. Good health
dc.titleThe Structure-Activity Relatıonships of Familiar Antiepileptic Drugs and Na+ Channels
dc.typeArticle
dspace.entity.typePublication
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