Novel tablet formulation of amorphous candesartan cilexetil solid dispersions involving P-gp inhibition for optimal drug delivery: <i>in vitro</i> and <i>in vivo</i> evaluation

Surampalli, Gurunath; Nanjwade, Basavaraj K.; Patil, P. A.; Chilla, Rakesh

doi:10.3109/10717544.2014.945017

Cited by 22 publications

(14 citation statements)

References 28 publications

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“…Finally, the mixture was compressed into convex faced tablets weighing 200 mg, with 5 mm diameter by a single punch tablet machine. The compression force and time was 20 kN and 32 s, respectively (Surampalli & Nanjwade, 2014).…”

Section: Preparation Of Sim/soluplus Sd-t Via Direct Compression Methodsmentioning

confidence: 99%

Extruded Soluplus/SIM as an oral delivery system: characterization, interactions,in vitroandin vivoevaluations

et al. 2014

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The aim of this study was to obtain a stable, amorphous solid dispersion (SD) with Soluplus, prepared by hot-melt extrusion (HME) as an effective and stable oral delivery system to improve the physical stability and bioavailability of the poorly water-soluble simvastatin (SIM), a drug with relatively low Tg. The drug was proved to be miscible with Soluplus by calculation and measurements. The solubility, dissolution, thermal characteristics, interactions and physical stability of the SIM/Soluplus SDs were investigated. The crystal state of simvastatin in the SD was found to change from crystalline to amorphous form during the HME process and also hydrogen bonds were observed between SIM and the extruded Soluplus. The phase solubility showed the solubilization effect of Soluplus was strong and spontaneous. The equilibrium solubility illustrated that Soluplus/SIM SDs gained much higher solubility than its corresponding physical mixtures (PMs). Both of the dissolution profiles and in-vivo performance showed that the SIM/Soluplus SD obtained a marked enhancement, compared with the PM. There was a little change in the SIM/Soluplus SD during a 3-month storage period (40 C, 75%), indicating the good physicochemical stability. The extruded Soluplus system prepared by HME is a good alternative for the water-insoluble SIM to improve the stability and bioavailability.

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Section: Preparation Of Sim/soluplus Sd-t Via Direct Compression Methodsmentioning

confidence: 99%

Extruded Soluplus/SIM as an oral delivery system: characterization, interactions,in vitroandin vivoevaluations

et al. 2014

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“…Optimasi MM2 Minimization (121)(122)(123)(124)(125)(126)(127)(128)(129)(130)(131)(132)(133)(134)(135) 2. Optimasi MM2 Dynamics (136)(137)(138)(139)(140) 3. Optimasi MM2 Properties (30; [141][142][143][144][145]…”

Section: Optimasi Molekul H3aso4 Menggunakan Molecular Mechanic (Mm2)unclassified

Asam Arsenat (H3AsO4) : Analisis Molekular dan Karakteristik Senyawa

Hakimi¹,

Zainul²

2019

Preprint

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Asam arsenat merupakan senyawa kimia dengan rumus molekul H3AsO4. Asam arsenat juga bisa dikenal dengan rumus molekul AsO(OH)3. Asam yang tidak berwarna ini merupakan analog asam fosfat, garam arsenat dan fosfat sendiri memiliki reaksi yang serupa. Asam arsenat masih belum diisolasi dan hanya dapat ditemukan di dalam larutan dan disanalah asam ini sangat terionisasi. Bentuk hemihidratnya (H3AsO4•1⁄2 H2O) dapat membentuk kristal yang stabil. Penelitian ini bertujuan untuk menganalisis struktur, interaksi molecular dan MM2 terhadap molekul asam arsenat. Metoda yang digunakan yaitu penelusuran literatur dengan Endnote X7, metode pemodelan dengan menggunakan software ChemOffice 15.0, dan juga perhitungan matematis. Pada dasarnya untuk menemukan literasi jurnal yang bagus digunakanlah aplikasi Endnote X7 yang dijelaskan melalui fishbone state of art. Analisis 2D struktur asam format menggunakan aplikasi chemdraw ultra dan analisis 3D struktur asam format menggunakan aplikasi chembio 3D. Asam arsenat juga memiliki total energi yang dapat diketahui menggunakan Chemoffice 15.0 yaitu sebesar 85.2948 kcal/mol, streach 0.0516, bend 66.4930, streach-bend -0.1025, torsion 23.4363, dan dipol-dipol -2.0437. Untuk mengetahui nilai viskositas, gerakan ion, kecepatan hanyut digunakan pengolahan data dan review jurnal mengenai asam arsenat. Asam arsenat memiliki nilai ∆fG -766.75, ∆fH -903.45, dan So 183.07 serta nilai kecepatan hanyut sebesar 3,628 V/cm setelah dihitung menggunakan rumus.

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“…Candesartan cilexetil low solubility, combined with its efflux transport by the intestinal P-glycoprotein and its vulnerability to enzymatic degradation in small intestine contribute to the observed low oral bioavailability [7][8][9]. Recently, an improvement of candesartan cilexetil oral bioavailability in rabbits has been demonstrated by using naringin as a P-gp inhibitor [10]. After absorption, candesartan is mainly excreted unchanged in urine and feces (by biliary excretion).…”

Section: Introductionmentioning

confidence: 99%

Candesartan Cilexetil In Vitro–In Vivo Correlation: Predictive Dissolution as a Development Tool

et al. 2020

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The main objective of this investigation was to develop an in vitro–in vivo correlation (IVIVC) for immediate release candesartan cilexetil formulations by designing an in vitro dissolution test to be used as development tool. The IVIVC could be used to reduce failures in future bioequivalence studies. Data from two bioequivalence studies were scaled and combined to obtain the dataset for the IVIVC. Two-step and one-step approaches were used to develop the IVIVC. Experimental solubility and permeability data confirmed candesartan cilexetil. Biopharmaceutic Classification System (BCS) class II candesartan average plasma profiles were deconvoluted by the Loo-Riegelman method to obtain the oral fractions absorbed. Fractions dissolved were obtained in several conditions in USP II and IV apparatus and the results were compared calculating the f2 similarity factor. Levy plot was constructed to estimate the time scaling factor and to make both processes, dissolution and absorption, superimposable. The in vitro dissolution experiment that reflected more accurately the in vivo behavior of the products of candesartan cilexetil employed the USP IV apparatus and a three-step pH buffer change, from 1.2 to 4.5 and 6.8, with 0.2% of Tween 20. This new model was able to predict the in vivo differences in dissolution and it could be used as a risk-analysis tool for formulation selection in future bioequivalence trials.

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Novel tablet formulation of amorphous candesartan cilexetil solid dispersions involving P-gp inhibition for optimal drug delivery: in vitro and in vivo evaluation

Cited by 22 publications

References 28 publications

Extruded Soluplus/SIM as an oral delivery system: characterization, interactions,in vitroandin vivoevaluations

Extruded Soluplus/SIM as an oral delivery system: characterization, interactions,in vitroandin vivoevaluations

Asam Arsenat (H3AsO4) : Analisis Molekular dan Karakteristik Senyawa

Candesartan Cilexetil In Vitro–In Vivo Correlation: Predictive Dissolution as a Development Tool

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