Measurement of density variations in tablets using X-ray computed tomography

Sinka, I.C.; Burch, S. F.; Tweed, J. H.; Cunningham, J. C.

doi:10.1016/j.ijpharm.2003.11.022

Cited by 174 publications

(94 citation statements)

References 11 publications

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“…Object image is then subtracted from this empty image to resume the final image. The reasons for this correction are that: i) X-ray detectors are uneven in intensity and often more sensitive towards the centre and, ii) X-ray beam is also nonuniform, often being stronger in the centre [5]. The final images are obtained in gray scale, but it also could be manipulated by using software techniques to produce binary or multiple-colored images.…”

Section: Resultsmentioning

confidence: 99%

“…In recent years, many non-conventional uses of CT has been introduced. Some of theses, for instance, applied to pharmaceutical industry, are: a) use of X-ray tomography to study the porosity and morphology of granules [4], b) measurement of density variation in tablets [5] and c) studies of internal structures of solid dosage forms [6]. This new approach to study properties of tablets, powders, granulations and liquid filled gelatin capsule is very suitable, first, because CT could generate information that traditional technologies used in this kind of analysis could not, such as: density distribution of internal structures without destroying the sample, tablet dimensions and integrity, pore size distribution, particle shape information, investigation of official and unofficial (counterfeit) copies of solid dosage forms and, second, because CT is a nondestructive technique, allowing the use of solid dosage forms in others analysis and also requires no specimen preparation.…”

Section: Introductionmentioning

confidence: 99%

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Non-Conventional Applications of Computerized Tomography: Analysis of Solid Dosage Forms Produced by Pharmaceutical Industry

Oliveira¹,

Martins²

2010

AIP Conference Proceedings

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Abstract. X-ray computed tomography (CT) refers to the cross-sectional imaging of an object measuring the transmitted radiation at different directions. In this work, we describe a nonconventional application of computerized tomography: visualization and improvements in the understanding of some internal structural features of solid dosage forms. A micro-CT X-ray scanner, with a minimum resolution of 30 µm was used to characterize some pharmaceutical tablets, granules, controlled-release osmotic tablet and liquid-filled soft-gelatin capsules. The analysis presented in this work are essentially qualitative, but quantitative parameters, such as porosity, density distribution, tablets dimensions, etc. could also be obtained using the related CT techniques.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Non-Conventional Applications of Computerized Tomography: Analysis of Solid Dosage Forms Produced by Pharmaceutical Industry

Oliveira¹,

Martins²

2010

AIP Conference Proceedings

View full text Add to dashboard Cite

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“…The sample is placed on a precision turntable between a high power X-ray source and a detector array (line or area array), which is used to measure the intensities of the diverging X-ray beam transmitted through the sample (12,15). Multiple attenuation coefficient values, which correlate to the degree of attenuation of the Xrays, are obtained as the sample is rotated relative to the Xray beam (to obtain multiple sets of attenuation coefficients from different viewing angles) (12,16,17). This raw data can be converted to pixel greyscale data, which a mathematical algorithm can translate into two-dimensional grey-scale radiograph or projection images (12,15).…”

Section: X-ray Computed Microtomographymentioning

confidence: 99%

“…Multiple attenuation coefficient values, which correlate to the degree of attenuation of the Xrays, are obtained as the sample is rotated relative to the Xray beam (to obtain multiple sets of attenuation coefficients from different viewing angles) (12,16,17). This raw data can be converted to pixel greyscale data, which a mathematical algorithm can translate into two-dimensional grey-scale radiograph or projection images (12,15). Furthermore, the computer system can be calibrated so that values are assigned to certain materials.…”

Section: X-ray Computed Microtomographymentioning

confidence: 99%

Microstructural Analysis of Porous Composite Materials: Dynamic Imaging of Drug Dissolution and Diffusion Through Porous Matrices

Young

Nguyen

Jones

et al. 2008

AAPS J

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“…Synchrotron radiation X-ray computed microtomography (SR-μCT) has previously been used to explore the microstructural characteristics of tablet formulations indicating the fracture patterns of tablets prepared under different compositions and compaction pressures and to determine the density distribution of compressed dosage forms (20)(21)(22)(23)(24).…”

Section: Introductionmentioning

confidence: 99%

Quantification of Swelling and Erosion in the Controlled Release of a Poorly Water-Soluble Drug Using Synchrotron X-ray Computed Microtomography

Yin

Guo

et al. 2013

AAPS J

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Abstract. The hydration layer plays a key role in the controlled drug release of gel-forming matrix tablets. For poorly water-soluble drugs, matrix erosion is considered as the rate limiting step for drug release. However, few investigations have reported on the quantification of the relative importance of swelling and erosion in the release of poorly soluble drugs, and three-dimensional (3D) structures of the hydration layer are poorly understood. Here, we employed synchrotron radiation X-ray computed microtomography with 9-μm resolution to investigate the hydration dynamics and to quantify the relative importance of swelling and erosion on felodipine release by a statistical model. The 3D structures of the hydration layer were revealed by the reconstructed 3D rendering of tablets. Twenty-three structural parameters related to the volume, the surface area (SA), and the specific surface area (SSA) for the hydration layer and the tablet core were calculated. Three dominating parameters, including SA and SSA of the hydration layer (SA hydration layer and SSA hydration layer ) and SA of the glassy core (SA glassy core ), were identified to establish the statistical model. The significance order of independent variables was SA hydration layer > SSA hydration layer > SA glassy core , which quantitatively indicated that the release of felodipine was dominated by a combination of erosion and swelling. The 3D reconstruction and structural parameter calculation methods in our study, which are not available from conventional methods, are efficient tools to quantify the relative importance of swelling and erosion in the controlled release of poorly soluble drugs from a structural point of view.

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Measurement of density variations in tablets using X-ray computed tomography

Cited by 174 publications

References 11 publications

Non-Conventional Applications of Computerized Tomography: Analysis of Solid Dosage Forms Produced by Pharmaceutical Industry

Non-Conventional Applications of Computerized Tomography: Analysis of Solid Dosage Forms Produced by Pharmaceutical Industry

Microstructural Analysis of Porous Composite Materials: Dynamic Imaging of Drug Dissolution and Diffusion Through Porous Matrices

Quantification of Swelling and Erosion in the Controlled Release of a Poorly Water-Soluble Drug Using Synchrotron X-ray Computed Microtomography

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