Bioavailability study of Theo-dur tablets in the fasted cannulated dog

Jiahorng Liaw; Avri Rubinstein; Joseph R. Robinson

doi:10.1016/0378-5173(90)90084-H

Bioavailability study of Theo-dur tablets in the fasted cannulated dog

Jiahorng Liaw, Avri Rubinstein, Joseph R. Robinson

Research output: Contribution to journal › Article › peer-review

15 Citations (Scopus)

Abstract

The present study uses the cannulated dog to verify the major elements of gastrointestinal (GI) motility affecting the performance of oral sustained release dosage forms. It appears that the residence time of a Theo-dur tablet in the fasted canine stomach and small intestine is dictated by the phasic activity of the motility pattern at the time of ingestion. The tablet does not disintegrate in vivo but undergoes surface erosion. Onset of tablet discharge corresponded with late phase II and phase III activity. The discharged eroded tablet was entrapped within mucus plugs. Mucus may play a significant role in the dissolution of administered tablets. There is little variability in the duodenal and ileal effluent pH, observed after onset of Theo-dur tablet discharge.

Original language	English
Pages (from-to)	105-114
Number of pages	10
Journal	International Journal of Pharmaceutics
Volume	59
Issue number	2
DOIs	https://doi.org/10.1016/0378-5173(90)90084-H
Publication status	Published - Mar 20 1990
Externally published	Yes

Keywords

Cannulated dog
Deconvolution method
Fasted state
Gastrointestinal motility
Mucus
Theo-dur tablet
Theophylline

ASJC Scopus subject areas

Pharmaceutical Science

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10.1016/0378-5173(90)90084-H

Cite this

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title = "Bioavailability study of Theo-dur tablets in the fasted cannulated dog",

abstract = "The present study uses the cannulated dog to verify the major elements of gastrointestinal (GI) motility affecting the performance of oral sustained release dosage forms. It appears that the residence time of a Theo-dur tablet in the fasted canine stomach and small intestine is dictated by the phasic activity of the motility pattern at the time of ingestion. The tablet does not disintegrate in vivo but undergoes surface erosion. Onset of tablet discharge corresponded with late phase II and phase III activity. The discharged eroded tablet was entrapped within mucus plugs. Mucus may play a significant role in the dissolution of administered tablets. There is little variability in the duodenal and ileal effluent pH, observed after onset of Theo-dur tablet discharge.",

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AU - Liaw, Jiahorng

AU - Rubinstein, Avri

AU - Robinson, Joseph R.

PY - 1990/3/20

Y1 - 1990/3/20

N2 - The present study uses the cannulated dog to verify the major elements of gastrointestinal (GI) motility affecting the performance of oral sustained release dosage forms. It appears that the residence time of a Theo-dur tablet in the fasted canine stomach and small intestine is dictated by the phasic activity of the motility pattern at the time of ingestion. The tablet does not disintegrate in vivo but undergoes surface erosion. Onset of tablet discharge corresponded with late phase II and phase III activity. The discharged eroded tablet was entrapped within mucus plugs. Mucus may play a significant role in the dissolution of administered tablets. There is little variability in the duodenal and ileal effluent pH, observed after onset of Theo-dur tablet discharge.

AB - The present study uses the cannulated dog to verify the major elements of gastrointestinal (GI) motility affecting the performance of oral sustained release dosage forms. It appears that the residence time of a Theo-dur tablet in the fasted canine stomach and small intestine is dictated by the phasic activity of the motility pattern at the time of ingestion. The tablet does not disintegrate in vivo but undergoes surface erosion. Onset of tablet discharge corresponded with late phase II and phase III activity. The discharged eroded tablet was entrapped within mucus plugs. Mucus may play a significant role in the dissolution of administered tablets. There is little variability in the duodenal and ileal effluent pH, observed after onset of Theo-dur tablet discharge.

KW - Cannulated dog

KW - Deconvolution method

KW - Fasted state

KW - Gastrointestinal motility

KW - Mucus

KW - Theo-dur tablet

KW - Theophylline

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Bioavailability study of Theo-dur tablets in the fasted cannulated dog

Abstract

Keywords

ASJC Scopus subject areas

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