FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2972507338> ?p ?o ?g. }

• W2972507338 endingPage "235" @default.
• W2972507338 startingPage "230" @default.
• W2972507338 abstract "Objective: In the present work, the main objective was to develop bilayer extended release matrix tablets of etoricoxib by providing a loading dose followed by maintenance dose that expected to improve the therapeutic efficacy of the medication with less toxic effect.&#x0D; Methods: Bilayer tablets of etoricoxib was developed successfully with the meticulous proportion of release controlling Hydroxy propyl methyl cellulose K100 (HPMC K100) and lactose. The tablets were prepared by wet granulation technique. Granules for immediate layer and extended layer for different formulations were prepared separately. The formulations were developed and evaluations were performed to examine the parameters that affect the in vitro performance of the tablets. The drug-excipient compatibility was ensured by Fourier transform infrared spectroscopy (FTIR) study.&#x0D; Results: The values of physical parameters of all formulations were found within appreciable limit. Formulation containing HPMC K 100 and lactose in the proportion of 2:1 in the extended release layer was able to release 26.22% of drug in 15 min and shown a steady release of drug for an extended period of 12 h. The dissolution data was put in Korsemeyer–Peppas model in order to find out n value, which describes the drug release mechanism. The n-value of different formulations were found to be variable. The Fourier transform infrared spectroscopy (FTIR) study revealed absence of any other new peaks and also no differences in the positions of the absorption bands in the bilayer tablet F8 that indicate the lack of significant interactions between etoricoxib and other excipients.&#x0D; Conclusion: It had been concluded that once daily immediate-and extended release bilayer tablet of etoricoxib can be formulated with profound physical characteristics and dissolution properties. This resulted in reducing the daily dose and thus minimise the cardiovascular toxicity of etoricoxib." @default.
• W2972507338 created "2019-09-19" @default.
• W2972507338 creator A5041262355 @default.
• W2972507338 creator A5050010289 @default.
• W2972507338 date "2019-07-25" @default.
• W2972507338 modified "2023-09-25" @default.
• W2972507338 title "ONCE DAILY IMMEDIATE-AND EXTENDED-RELEASE BILAYER TABLETS OF ETORICOXIB: A STUDY ON THE RELEASE KINETICS" @default.
• W2972507338 doi "https://doi.org/10.22159/ijap.2019v11i5.31638" @default.
• W2972507338 hasPublicationYear "2019" @default.
• W2972507338 type Work @default.
• W2972507338 sameAs 2972507338 @default.
• W2972507338 citedByCount "2" @default.
• W2972507338 countsByYear W29725073382020 @default.
• W2972507338 countsByYear W29725073382022 @default.
• W2972507338 crossrefType "journal-article" @default.
• W2972507338 hasAuthorship W2972507338A5041262355 @default.
• W2972507338 hasAuthorship W2972507338A5050010289 @default.
• W2972507338 hasBestOaLocation W29725073381 @default.
• W2972507338 hasConcept C127413603 @default.
• W2972507338 hasConcept C159985019 @default.
• W2972507338 hasConcept C160892712 @default.
• W2972507338 hasConcept C178790620 @default.
• W2972507338 hasConcept C185592680 @default.
• W2972507338 hasConcept C192157962 @default.
• W2972507338 hasConcept C192562407 @default.
• W2972507338 hasConcept C2776214540 @default.
• W2972507338 hasConcept C2778724459 @default.
• W2972507338 hasConcept C3019981671 @default.
• W2972507338 hasConcept C33923547 @default.
• W2972507338 hasConcept C41625074 @default.
• W2972507338 hasConcept C42360764 @default.
• W2972507338 hasConcept C43617362 @default.
• W2972507338 hasConcept C55493867 @default.
• W2972507338 hasConcept C88380143 @default.
• W2972507338 hasConcept C88463166 @default.
• W2972507338 hasConceptScore W2972507338C127413603 @default.
• W2972507338 hasConceptScore W2972507338C159985019 @default.
• W2972507338 hasConceptScore W2972507338C160892712 @default.
• W2972507338 hasConceptScore W2972507338C178790620 @default.
• W2972507338 hasConceptScore W2972507338C185592680 @default.
• W2972507338 hasConceptScore W2972507338C192157962 @default.
• W2972507338 hasConceptScore W2972507338C192562407 @default.
• W2972507338 hasConceptScore W2972507338C2776214540 @default.
• W2972507338 hasConceptScore W2972507338C2778724459 @default.
• W2972507338 hasConceptScore W2972507338C3019981671 @default.
• W2972507338 hasConceptScore W2972507338C33923547 @default.
• W2972507338 hasConceptScore W2972507338C41625074 @default.
• W2972507338 hasConceptScore W2972507338C42360764 @default.
• W2972507338 hasConceptScore W2972507338C43617362 @default.
• W2972507338 hasConceptScore W2972507338C55493867 @default.
• W2972507338 hasConceptScore W2972507338C88380143 @default.
• W2972507338 hasConceptScore W2972507338C88463166 @default.
• W2972507338 hasLocation W29725073381 @default.
• W2972507338 hasOpenAccess W2972507338 @default.
• W2972507338 hasPrimaryLocation W29725073381 @default.
• W2972507338 hasRelatedWork W2012902082 @default.
• W2972507338 hasRelatedWork W2291923075 @default.
• W2972507338 hasRelatedWork W2389250902 @default.
• W2972507338 hasRelatedWork W2551743698 @default.
• W2972507338 hasRelatedWork W2592631860 @default.
• W2972507338 hasRelatedWork W2972507338 @default.
• W2972507338 hasRelatedWork W3165822627 @default.
• W2972507338 hasRelatedWork W4377247675 @default.
• W2972507338 hasRelatedWork W2182294410 @default.
• W2972507338 hasRelatedWork W2556848074 @default.
• W2972507338 isParatext "false" @default.
• W2972507338 isRetracted "false" @default.
• W2972507338 magId "2972507338" @default.
• W2972507338 workType "article" @default.