Simulating the hydrodynamic conditions in the united states pharmacopeia paddle dissolution apparatus

McCarthy, Leonard; Kosiol, Carolin; Healy, Anne Marie; Bradley, Geoff; Sexton, James; Corrigan, Owen I.

doi:10.1208/pt040222

Cited by 86 publications

(89 citation statements)

References 14 publications

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“…Drug release of a poorly soluble drug like EFV, as used in the study, is usually driven more by the medium than by the formulation ingredients. Discriminatory dissolution profiles are highly desirable for distinguishing between products showing differences in pharmaceutical attributes (formulation or manufacturing process differences) as is the case in the present study, wherein the difference in formulation was only with respect to the disintegrant used (10)(11)(12)(13). Figure 1 shows the dissolution profile of 600-mg EFV tablet in water containing different concentrations of SLS containing CP as disintegrant.…”

Section: In Vitro Dissolution Studiesmentioning

confidence: 89%

Impact of superdisintegrants on efavirenz release from tablet formulations

Yelchuri

Balasubramaniam

K³

et al. 2010

Acta Pharmaceutica

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EFV is a non-nucleoside reverse transcriptase inhibitor and is used as part of the highly active antiretroviral therapy for the treatment of human immunodeficiency virus type 1 (HIV) infection. It is also used in combination with other antiretroviral agents as part of an expanded post-exposure prophylaxis regimen to prevent HIV transmission for those exposed to materials associated with a high risk of HIV transmission.EFV has poor aqueous solubility and is a BCS class II drug (1). EFV tablets of 600 mg are available, while lower doses (50, 100 and 200 mg) are generally available as capsules and are prepared by a wet granulation process (2, 3). 185Acta Pharm. 60 (2010) [185][186][187][188][189][190][191][192][193][194][195] Original research paper DOI: 10.2478/v10007-010-0019-6 Impact of superdisintegrants on efavirenz release from tablet formulations Efavirenz (EFV) tablets of different doses were prepared by a wet granulation process using different superdisintegrants such as crosscarmellose sodium (CCS), sodium starch glycollate (SSG) and crosspovidone (CP) to evaluate the role of different disintegrants on the in vitro release of EFV. Further, the mode of addition of disintegrants on EFV dissolution from tablets containing 600 mg of the drug was evaluated by incorporating the disintegrants extragranularly (EG), intragranularly (IG) or distributing them equally (IG and EG). In vitro dissolution of the prepared tablets was conducted using the recommended medium and a dissolution medium developed in-house, which had the ability to discriminate between the formulations.The t 50 and t 80 values were indicative of the fact that the drug release was faster from tablet formulations containing CP. CP was able to release the drug faster than the other two disintegrants in both dissolution media and the drug release was unaffected by the mode of CP addition.Keywords: efavirenz, superdisintegrants, granulation * Correspondence; e-mail: rajeshyelchuri@rediffmail.com Brought to you by | MIT Libraries Authenticated Download Date | 5/12/18 2:48 PM Superdisintegrants generally improve disintegration efficiency compared to traditional disintegrants. They are generally used at low levels in solid dosage forms, typically 1-10 % of mass relative to the total mass of the dosage unit (4). Examples of superdisintegrants are crosscarmellose sodium (CCS), sodium starch glycollate (SSG) and crosspovidone (CP), which are cross-linked cellulose, a cross-linked starch and a cross--linked polymer (polyvinyl pyrrolidone), respectively. Wet granulation is one of the frequently used techniques to prepare blends to be compressed into tablets. The disintegrant can be incorporated in the blend before granulation, referred to as intragranular addition (IG), or after granulation, referred to as extragranular addition (EG), or it can be distributed both intra and extragranularly. EXPERIMENTAL MaterialsEfavirenz (Aurbindo Pharma Ltd., India) was purchased from the source indicated. Crosscarmellose sodium (Ac-di-sol ® , FMC biopolymer) and SS...

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Section: In Vitro Dissolution Studiesmentioning

confidence: 89%

Impact of superdisintegrants on efavirenz release from tablet formulations

Yelchuri

Balasubramaniam

K³

et al. 2010

Acta Pharmaceutica

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“…Differences in the dimensions result in measurable differences in both the paddle tip-vessel wall clearance and in the volume of dissolution media surrounding the paddle. It has been shown that heterogeneous shear rates exist in the hemispheric region of the dissolution vessel (10,11). Given the differences in both the paddle-vessel wall clearance and in the volume of dissolution media surrounding the paddle, hydrodynamics in the hemispheric region of the vessel could be influenced by variability of the dimensions of this critical region of the dissolution vessel.…”

Section: Discussionmentioning

confidence: 99%

Evaluation of Glass Dissolution Vessel Dimensions and Irregularities

Liddell¹,

Deng²,

Brown³

et al. 2007

Dissolution Technol.

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“…Recirculation loops have been identified in both the upper and lower sections of the vessel, with a weak positive axial flow under the impeller in the center of lower part of the vessel. Overall fluid velocity values and shear rates in the vessel base are very low, especially at the center of the vessel base compared to other regions of the vessel (13,21,(24)(25)(26)(27).…”

Section: General Flow Featuresmentioning

confidence: 94%

“…Under the standard operating conditions mandated by the dissolution test procedure, with no tablets present in the vessel, the shear strain environment in USP Apparatus 2 is highly heterogeneous with strain rate and fluid velocities varying significantly along the vessel base (21,(24)(25)(26)(27)29). These heterogeneous hydrodynamic conditions are present in the vessel base region where a dosage form is likely to be located.…”

Section: Hydrodynamics In the Lower Hemispherical Section Of The Vesselmentioning

confidence: 99%

Characterization and Simulation of Hydrodynamics in the Paddle, Basket and Flow-Through Dissolution Testing Apparatuses - A Review

Todaro¹,

Pearsons²,

Grove³

et al. 2017

Dissolution Technol.

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Fluid velocity local to the dissolving surface will affect the dissolution rate. It is difficult to anticipate what local fluid velocities are present within compendial dissolution apparatuses from set flow rates or stirring rates. A range of qualitative and quantitative velocimetric techniques are available to assess and characterize hydrodynamics. These methods are frequently used in combination with computational fluid dynamics simulations to characterize and simulate hydrodynamics. Dosage form location and motion varies between apparatuses, and the presence of the dosage form itself can impact local hydrodynamics. Each apparatus described has identified hydrodynamic features which may also vary with agitation rate. This review describes the methods used to simulate and characterize hydrodynamics and summarizes some of the main findings from studies investigating hydrodynamics in the paddle, basket, and flowthrough dissolution apparatuses.

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Simulating the hydrodynamic conditions in the united states pharmacopeia paddle dissolution apparatus

Cited by 86 publications

References 14 publications

Impact of superdisintegrants on efavirenz release from tablet formulations

Impact of superdisintegrants on efavirenz release from tablet formulations

Evaluation of Glass Dissolution Vessel Dimensions and Irregularities

Characterization and Simulation of Hydrodynamics in the Paddle, Basket and Flow-Through Dissolution Testing Apparatuses - A Review

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