FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2789119707> ?p ?o ?g. }

• W2789119707 endingPage "0084" @default.
• W2789119707 startingPage "0065" @default.
• W2789119707 abstract "Quantitative structure activity relationship study (QSAR) and molecular docking were used to design and virtually screen some new N-benzylacetamide derivatives for their ability to inhibit ?-amino butyrate-aminotransferase. Ninety compounds with anticonvulsant activity against maximal electroshock induced seizures were used for QSAR study. B3LYP/6-31G** quantum mechanical method was employed to optimize/minimize the molecular structure of these compounds. Genetic Function Algorithm (GFA) method was used to develop the QSAR models. Each model gave an octa-parametric equation with good statistical qualities (R2 ranged from 0.823 to 0.893, Q2 from 0.772 to 0.854, F from 36.53 to 37.10, R2pred(test) from 0.768 to 0.893). Information obtained from the parameter contained in the model suggested that increasing the molecular mass and linearity of molecule would lead to increase in anticonvulsant activity of studied compounds. These informed the design and virtual screening of 118 new N-benzylacetamide derivatives using 2-acetamido-N-benzyl-2-(5-methylfuran-2-yl)acetamides as the template. The designed molecules were docked with ?-amino butyrate-aminotransferase (GABA_AT; PDB: 1OHV) using Internal Coordinate Mechanics Program (ICM-pro 3.8-3). The binding affinity of the designed compounds with GABA_AT were comparable to that of 4-aminohex-5-enoic acid (vigabatrin) and 3, 3-diphenylpyrrolidine-2, 5-dione (phenytoin) and 5H-dibenzo [b,f]azepine-5-carboxamide (carbamazepine), which are known inhibitors of GABA_AT. Therefore, the designed molecules have potential as inhibitors of GABA_AT and consequently as anticonvulsant agent." @default.
• W2789119707 created "2018-03-06" @default.
• W2789119707 creator A5017427535 @default.
• W2789119707 creator A5032573298 @default.
• W2789119707 creator A5033339409 @default.
• W2789119707 creator A5046349695 @default.
• W2789119707 date "2018-01-16" @default.
• W2789119707 modified "2023-10-13" @default.
• W2789119707 title "QSAR and molecular docking based design of some n-benzylacetamide as ?-aminobutyrate-aminotransferase inhibitors" @default.
• W2789119707 doi "https://doi.org/10.18540/jcecvl4iss1pp0065-0084" @default.
• W2789119707 hasPublicationYear "2018" @default.
• W2789119707 type Work @default.
• W2789119707 sameAs 2789119707 @default.
• W2789119707 citedByCount "10" @default.
• W2789119707 countsByYear W27891197072019 @default.
• W2789119707 countsByYear W27891197072020 @default.
• W2789119707 countsByYear W27891197072021 @default.
• W2789119707 countsByYear W27891197072022 @default.
• W2789119707 countsByYear W27891197072023 @default.
• W2789119707 crossrefType "journal-article" @default.
• W2789119707 hasAuthorship W2789119707A5017427535 @default.
• W2789119707 hasAuthorship W2789119707A5032573298 @default.
• W2789119707 hasAuthorship W2789119707A5033339409 @default.
• W2789119707 hasAuthorship W2789119707A5046349695 @default.
• W2789119707 hasBestOaLocation W27891197071 @default.
• W2789119707 hasConcept C147597530 @default.
• W2789119707 hasConcept C159110408 @default.
• W2789119707 hasConcept C164126121 @default.
• W2789119707 hasConcept C178790620 @default.
• W2789119707 hasConcept C185592680 @default.
• W2789119707 hasConcept C2777939525 @default.
• W2789119707 hasConcept C32909587 @default.
• W2789119707 hasConcept C41685203 @default.
• W2789119707 hasConcept C71240020 @default.
• W2789119707 hasConcept C71924100 @default.
• W2789119707 hasConceptScore W2789119707C147597530 @default.
• W2789119707 hasConceptScore W2789119707C159110408 @default.
• W2789119707 hasConceptScore W2789119707C164126121 @default.
• W2789119707 hasConceptScore W2789119707C178790620 @default.
• W2789119707 hasConceptScore W2789119707C185592680 @default.
• W2789119707 hasConceptScore W2789119707C2777939525 @default.
• W2789119707 hasConceptScore W2789119707C32909587 @default.
• W2789119707 hasConceptScore W2789119707C41685203 @default.
• W2789119707 hasConceptScore W2789119707C71240020 @default.
• W2789119707 hasConceptScore W2789119707C71924100 @default.
• W2789119707 hasIssue "1" @default.
• W2789119707 hasLocation W27891197071 @default.
• W2789119707 hasOpenAccess W2789119707 @default.
• W2789119707 hasPrimaryLocation W27891197071 @default.
• W2789119707 hasRelatedWork W1980293288 @default.
• W2789119707 hasRelatedWork W2001717463 @default.
• W2789119707 hasRelatedWork W2016318508 @default.
• W2789119707 hasRelatedWork W2024472470 @default.
• W2789119707 hasRelatedWork W2069492452 @default.
• W2789119707 hasRelatedWork W2148380874 @default.
• W2789119707 hasRelatedWork W2168796376 @default.
• W2789119707 hasRelatedWork W2169688334 @default.
• W2789119707 hasRelatedWork W2950397829 @default.
• W2789119707 hasRelatedWork W2952072599 @default.
• W2789119707 hasVolume "4" @default.
• W2789119707 isParatext "false" @default.
• W2789119707 isRetracted "false" @default.
• W2789119707 magId "2789119707" @default.
• W2789119707 workType "article" @default.