FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4368360680> ?p ?o ?g. }

• W4368360680 endingPage "7" @default.
• W4368360680 startingPage "1" @default.
• W4368360680 abstract "Coronavirus, an extremely contagious infections disease had a harmful effect on the world's population. It is a family of enveloped, single-stranded, positive-strand RNA viruses of Nidovirales order belongs to coroviridae family. At present, worldwide several lakhs of deaths and several billions of infections have been reported. Hence, the focus of the present study was to assess the SARS-CoV-2 enzyme inhibitory potential of certain commercially available terpenoids using Lamarckian genetic algorithm as a working principle and molecular dynamic studies was also performed. AutoDock 4.2 software was used to perform the computational docking calculations of terpenoids against SARS-CoV-2 enzyme. The terpenoids such as, Andrographolide, Betulonic acid, Erythrodiol, Friedelin, Mimuscopic acid, Moronic acid, and Retinol were selected based on the drug likeness properties. Remdesivir a well-known anti-viral drug was selected as the standard drug. Molecular dynamic simulation studies were carried using Desmond module of Schrodinger Suite. In the current study we observed that, Friedelin was exhibited excellent SARS-CoV-2 enzyme inhibitory potential than the standard drug and other selected terpenoids. Friedelin and the standard Remdesivir was undergone the molecular dynamic studies and Friedelin showed a good number of hydrogen bonds over the simulation time of 100 ns. Based on the in silico computational evaluation, it can be concluded that Friedelin could be worthwhile terpenoid against SARS-CoV-2 spike protein. A further study on Friedelin is required to develop a potential chemical entity against the management of COVID disease.Communicated by Ramaswamy H. Sarma." @default.
• W4368360680 created "2023-05-05" @default.
• W4368360680 creator A5022192939 @default.
• W4368360680 creator A5029491996 @default.
• W4368360680 creator A5032628515 @default.
• W4368360680 creator A5089380977 @default.
• W4368360680 date "2023-05-03" @default.
• W4368360680 modified "2023-09-25" @default.
• W4368360680 title "<i>In silico</i> evaluation of some commercially available terpenoids as spike glycoprotein of SARS-CoV-2 – inhibitors using molecular dynamic approach" @default.
• W4368360680 cites W1031578623 @default.
• W4368360680 cites W1990194768 @default.
• W4368360680 cites W1997815103 @default.
• W4368360680 cites W2045519806 @default.
• W4368360680 cites W2046696212 @default.
• W4368360680 cites W2059013803 @default.
• W4368360680 cites W2097780534 @default.
• W4368360680 cites W2102380386 @default.
• W4368360680 cites W2105668062 @default.
• W4368360680 cites W2131988685 @default.
• W4368360680 cites W2135904340 @default.
• W4368360680 cites W2152630148 @default.
• W4368360680 cites W2171268876 @default.
• W4368360680 cites W253217195 @default.
• W4368360680 cites W2552506015 @default.
• W4368360680 cites W2624810409 @default.
• W4368360680 cites W2752211047 @default.
• W4368360680 cites W2792254405 @default.
• W4368360680 cites W2927184371 @default.
• W4368360680 cites W2964640060 @default.
• W4368360680 cites W3006049090 @default.
• W4368360680 cites W3012818802 @default.
• W4368360680 cites W3028981427 @default.
• W4368360680 doi "https://doi.org/10.1080/07391102.2023.2201848" @default.
• W4368360680 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/37139540" @default.
• W4368360680 hasPublicationYear "2023" @default.
• W4368360680 type Work @default.
• W4368360680 citedByCount "0" @default.
• W4368360680 crossrefType "journal-article" @default.
• W4368360680 hasAuthorship W4368360680A5022192939 @default.
• W4368360680 hasAuthorship W4368360680A5029491996 @default.
• W4368360680 hasAuthorship W4368360680A5032628515 @default.
• W4368360680 hasAuthorship W4368360680A5089380977 @default.
• W4368360680 hasConcept C104317684 @default.
• W4368360680 hasConcept C107585567 @default.
• W4368360680 hasConcept C185592680 @default.
• W4368360680 hasConcept C206103511 @default.
• W4368360680 hasConcept C2775905019 @default.
• W4368360680 hasConcept C2781370004 @default.
• W4368360680 hasConcept C2908647359 @default.
• W4368360680 hasConcept C55493867 @default.
• W4368360680 hasConcept C71240020 @default.
• W4368360680 hasConcept C71924100 @default.
• W4368360680 hasConcept C86803240 @default.
• W4368360680 hasConcept C99454951 @default.
• W4368360680 hasConceptScore W4368360680C104317684 @default.
• W4368360680 hasConceptScore W4368360680C107585567 @default.
• W4368360680 hasConceptScore W4368360680C185592680 @default.
• W4368360680 hasConceptScore W4368360680C206103511 @default.
• W4368360680 hasConceptScore W4368360680C2775905019 @default.
• W4368360680 hasConceptScore W4368360680C2781370004 @default.
• W4368360680 hasConceptScore W4368360680C2908647359 @default.
• W4368360680 hasConceptScore W4368360680C55493867 @default.
• W4368360680 hasConceptScore W4368360680C71240020 @default.
• W4368360680 hasConceptScore W4368360680C71924100 @default.
• W4368360680 hasConceptScore W4368360680C86803240 @default.
• W4368360680 hasConceptScore W4368360680C99454951 @default.
• W4368360680 hasLocation W43683606801 @default.
• W4368360680 hasLocation W43683606802 @default.
• W4368360680 hasOpenAccess W4368360680 @default.
• W4368360680 hasPrimaryLocation W43683606801 @default.
• W4368360680 hasRelatedWork W1514968013 @default.
• W4368360680 hasRelatedWork W2018630221 @default.
• W4368360680 hasRelatedWork W2062559212 @default.
• W4368360680 hasRelatedWork W2078697172 @default.
• W4368360680 hasRelatedWork W2088062465 @default.
• W4368360680 hasRelatedWork W2091004783 @default.
• W4368360680 hasRelatedWork W2094117413 @default.
• W4368360680 hasRelatedWork W2340668334 @default.
• W4368360680 hasRelatedWork W2389396801 @default.
• W4368360680 hasRelatedWork W4301395162 @default.
• W4368360680 isParatext "false" @default.
• W4368360680 isRetracted "false" @default.
• W4368360680 workType "article" @default.