FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2807252714> ?p ?o ?g. }

• W2807252714 endingPage "68" @default.
• W2807252714 startingPage "62" @default.
• W2807252714 abstract "Nowadays, the market is flooded with combinations of drugs in various dosage forms, but there is a lack of official methods to quantify them. A single dissolution test method for the analysis of combined dosage form is preferred for simplification of quality control testing.If the developed dissolution medium mimics the biorelevant and discriminating dissolution procedure for drug products with limited drug aqueous solubility it is a useful tool for qualitative forecasting of the in vivo behavior of formulations.Dissolution profiles were evaluated for atorvastatin and fenofibrate in capsules, using a paddle-type United States Pharmacopeia dissolution apparatus in 900 mL of medium at 50 rpm and 37±0.5°C. The best medium was 900 mL of 0.5% w/v sodium lauryl sulfate. The cumulative % dissolution was more than 85% within 45 min for marketed tablets. The proposed dissolution test conditions have discriminative power, dissimilarity factor (f1) values are low (12-16%), and similarity (f2) factor values are also low (45-48%). Hence the use of 0.5% w/v sodium lauryl sulfate solution is justified.The dissolution method was validated (% relative standard deviation <2). To quantify both drugs simultaneously, a second derivative spectrophotometric method was established (λmax 281 nm and 296 nm, respectively, for atorvastatin and fenofibrate) in acetate buffer, pH 2.8 solution." @default.
• W2807252714 created "2018-06-13" @default.
• W2807252714 creator A5011402368 @default.
• W2807252714 creator A5025667117 @default.
• W2807252714 creator A5063643583 @default.
• W2807252714 creator A5068217919 @default.
• W2807252714 creator A5070465494 @default.
• W2807252714 creator A5074440572 @default.
• W2807252714 date "2019-03-01" @default.
• W2807252714 modified "2023-09-24" @default.
• W2807252714 title "Development of a Discriminative and Biorelevant Dissolution Test Method for Atorvastatin/Fenofibrate Combination with Appliance of Derivative Spectrophotometry" @default.
• W2807252714 cites W1522767714 @default.
• W2807252714 cites W2014152768 @default.
• W2807252714 cites W2091201593 @default.
• W2807252714 cites W2150933540 @default.
• W2807252714 cites W2223276738 @default.
• W2807252714 doi "https://doi.org/10.4274/tjps.77698" @default.
• W2807252714 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/7227977" @default.
• W2807252714 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/32454697" @default.
• W2807252714 hasPublicationYear "2019" @default.
• W2807252714 type Work @default.
• W2807252714 sameAs 2807252714 @default.
• W2807252714 citedByCount "3" @default.
• W2807252714 countsByYear W28072527142022 @default.
• W2807252714 countsByYear W28072527142023 @default.
• W2807252714 crossrefType "journal-article" @default.
• W2807252714 hasAuthorship W2807252714A5011402368 @default.
• W2807252714 hasAuthorship W2807252714A5025667117 @default.
• W2807252714 hasAuthorship W2807252714A5063643583 @default.
• W2807252714 hasAuthorship W2807252714A5068217919 @default.
• W2807252714 hasAuthorship W2807252714A5070465494 @default.
• W2807252714 hasAuthorship W2807252714A5074440572 @default.
• W2807252714 hasBestOaLocation W28072527141 @default.
• W2807252714 hasConcept C14029885 @default.
• W2807252714 hasConcept C155574463 @default.
• W2807252714 hasConcept C178790620 @default.
• W2807252714 hasConcept C185592680 @default.
• W2807252714 hasConcept C2777482532 @default.
• W2807252714 hasConcept C2778110834 @default.
• W2807252714 hasConcept C2778913249 @default.
• W2807252714 hasConcept C2781430271 @default.
• W2807252714 hasConcept C43617362 @default.
• W2807252714 hasConcept C71924100 @default.
• W2807252714 hasConcept C77281830 @default.
• W2807252714 hasConcept C88380143 @default.
• W2807252714 hasConcept C98274493 @default.
• W2807252714 hasConceptScore W2807252714C14029885 @default.
• W2807252714 hasConceptScore W2807252714C155574463 @default.
• W2807252714 hasConceptScore W2807252714C178790620 @default.
• W2807252714 hasConceptScore W2807252714C185592680 @default.
• W2807252714 hasConceptScore W2807252714C2777482532 @default.
• W2807252714 hasConceptScore W2807252714C2778110834 @default.
• W2807252714 hasConceptScore W2807252714C2778913249 @default.
• W2807252714 hasConceptScore W2807252714C2781430271 @default.
• W2807252714 hasConceptScore W2807252714C43617362 @default.
• W2807252714 hasConceptScore W2807252714C71924100 @default.
• W2807252714 hasConceptScore W2807252714C77281830 @default.
• W2807252714 hasConceptScore W2807252714C88380143 @default.
• W2807252714 hasConceptScore W2807252714C98274493 @default.
• W2807252714 hasIssue "1" @default.
• W2807252714 hasLocation W28072527141 @default.
• W2807252714 hasLocation W28072527142 @default.
• W2807252714 hasLocation W28072527143 @default.
• W2807252714 hasLocation W28072527144 @default.
• W2807252714 hasOpenAccess W2807252714 @default.
• W2807252714 hasPrimaryLocation W28072527141 @default.
• W2807252714 hasRelatedWork W2001381420 @default.
• W2807252714 hasRelatedWork W2013846109 @default.
• W2807252714 hasRelatedWork W2017450153 @default.
• W2807252714 hasRelatedWork W2049053648 @default.
• W2807252714 hasRelatedWork W2056735484 @default.
• W2807252714 hasRelatedWork W2807252714 @default.
• W2807252714 hasRelatedWork W3157785507 @default.
• W2807252714 hasRelatedWork W772928710 @default.
• W2807252714 hasRelatedWork W806858818 @default.
• W2807252714 hasRelatedWork W2181817826 @default.
• W2807252714 hasVolume "16" @default.
• W2807252714 isParatext "false" @default.
• W2807252714 isRetracted "false" @default.
• W2807252714 magId "2807252714" @default.
• W2807252714 workType "article" @default.