Literature DB >> 7667195

Regiospecific intestinal absorption of the HIV protease inhibitor L-735,524 in beagle dogs.

G Y Kwei1, L B Novak, L A Hettrick, E R Reiss, D Ostovic, A E Loper, C Y Lui, R J Higgins, I W Chen, J H Lin.   

Abstract

PURPOSE: To evaluate regional intestinal absorption and the feasibility of sustained release dosage form development for an HIV protease inhibitor, L-735,524,
METHODS: L-735,524 free base or sulfate salt was administered orally as suspension, solution or in solid dosage forms to fasted or fed Beagle dogs. Delayed-release dosage forms with "slow" or "fast" in vitro dissolution rates were evaluated in vivo to assess plasma concentration profiles. In addition, drug was administered directly into the jejunum or colon of animals, and drug concentrations determined in portal circulation to characterize absorption from these sites.
RESULTS: L-735,524 sulfate was well absorbed orally form a solution or capsule formulation if fasted animals' stomachs were preacidified with citric acid solution. A free base suspension, delivered in divided doses to fed animals, was also well absorbed. Prototype extended release dosage forms of L-735,524 produced a reduction in peak plasma levels but failed to prolong absorption and extend plasma concentrations compared to an immediate release capsule. Administration of L-735,524 sulfate solution (pH < 3) as bolus solution or by infusion into the jejunum resulted in rapid but incomplete absorption compared to oral gavage. The free base suspension (pH 6.5) delivered into jejunal or colonic regions did not produce measurable systemic plasma concentrations.
CONCLUSIONS: Extended release formulations did not prolong absorption of L-735,524 in dogs. Optimal L-735,524 absorption was dependent on solubility in an acidic environment in the duodenum.

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Year:  1995        PMID: 7667195     DOI: 10.1023/a:1016269206048

Source DB:  PubMed          Journal:  Pharm Res        ISSN: 0724-8741            Impact factor:   4.200


  7 in total

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2.  Chronic catheterization of the intestines and portal vein for absorption experimentation in beagle dogs.

Authors:  G Y Kwei; J R Gehret; L B Novak; M D Drag; T Goodwin
Journal:  Lab Anim Sci       Date:  1995-12

3.  L-735,524: an orally bioavailable human immunodeficiency virus type 1 protease inhibitor.

Authors:  J P Vacca; B D Dorsey; W A Schleif; R B Levin; S L McDaniel; P L Darke; J Zugay; J C Quintero; O M Blahy; E Roth
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4.  Effects of ranitidine and sucralfate on ketoconazole bioavailability.

Authors:  S C Piscitelli; T F Goss; J H Wilton; D T D'Andrea; H Goldstein; J J Schentag
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5.  High-performance liquid chromatographic determination of a potent and selective HIV protease inhibitor (L-735,524) in rat, dog and monkey plasma.

Authors:  I W Chen; K J Vastag; J H Lin
Journal:  J Chromatogr B Biomed Appl       Date:  1995-10-06

6.  Comparison of gastrointestinal pH in dogs and humans: implications on the use of the beagle dog as a model for oral absorption in humans.

Authors:  C Y Lui; G L Amidon; R R Berardi; D Fleisher; C Youngberg; J B Dressman
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Authors:  T L Russell; R R Berardi; J L Barnett; T L O'Sullivan; J G Wagner; J B Dressman
Journal:  Pharm Res       Date:  1994-01       Impact factor: 4.200

  7 in total
  6 in total

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5.  Dissolution improvement and the mechanism of the improvement from cocrystallization of poorly water-soluble compounds.

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Review 6.  Novel Nanotechnology-Based Approaches for Targeting HIV Reservoirs.

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Journal:  Polymers (Basel)       Date:  2022-07-29       Impact factor: 4.967

  6 in total

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