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Drug Marker Absorption in Relation to Pellet Size, Gastric Motility and Viscous Meals in Humans

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Abstract

Purpose. The objective of this study was to evaluate drug marker absorption in relation to the gastric emptying (GE) of 0.7 mm and 3.6 mm enteric coated pellets as a function of viscosity and the underlying gastric motility.

Methods. Twelve subjects were evaluated in a 3-way crossover study. 0.7 mm caffeine and 3.6 mm acetaminophen enteric coated pellets were concurrently administered with a viscous caloric meal at the levels of 4000, 6000 and 8000 cP. Gastric motility was simultaneously measured with antral manometry and compared to time events in the plasma profiles of the drug markers.

Results. Caffeine, from the 0.7 mm pellets, was observed significantly earlier in the plasma than acetaminophen, from the 3.6 mm pellets, at all levels of viscosity. Motility related size differentiated GE was consistently observed at all viscosity levels, however, less variability was observed with the 4000 cP meal. Specifically, the onset of absorption from the of 3.6 mm pellets correlated with the onset of Phase II fasted state contractions (r = 0.929, p < 0.01).

Conclusions. The timeframe of drug marker absorption and the onset of motility events were not altered within the range of viscosities evaluated. Rather, the differences in drug marker profiles from the non-digestible solids were most likely the result of the interaction between viscosity and motility influencing antral flow dynamics. The administration of the two sizes of pellets and a viscous caloric meal with subsequent monitoring of drug marker profiles is useful as a reference to assess the influence of motility patterns on the absorption profile of orally administered agents.

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Author notes

  1. Julie K. Rhie

    Present address: , NIH Bldg 29B Rm 2E06, Bethesda, Maryland, 20892

Authors and Affiliations

  1. College of Pharmacy, University of Michigan, Ann Arbor, Michigan

    Julie K. Rhie, Yayoi Hayashi, Lynda S. Welage, Jeremy Frens & Gordon L. Amidon

  2. College of Pharmacy, Nagoya City University, Nagoya, Japan

    Yayoi Hayashi

  3. Department of Pharmacy, University of Michigan Health Systems, Ann Arbor, Michigan

    Lynda S. Welage

  4. Pharmacia and Upjohn, Kalamazoo, Michigan

    Randy J. Wald & Gregory E. Amidon

  5. Department of Internal Medicine, Division of Gastroenterology and University of Michigan Medical School, University of Michigan Health Systems, Ann Arbor, Michigan

    Jeffrey L. Barnett

  6. NASA-Johnson Space Center, Houston, Texas

    Lakshmi Putcha

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  1. Julie K. Rhie
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  2. Yayoi Hayashi
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  9. Gordon L. Amidon
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Rhie, J.K., Hayashi, Y., Welage, L.S. et al. Drug Marker Absorption in Relation to Pellet Size, Gastric Motility and Viscous Meals in Humans. Pharm Res 15, 233–238 (1998). https://doi.org/10.1023/A:1011962501270

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