Literature DB >> 18349286

Comparative bioavailability of sulindac in capsule and tablet formulations.

Joel M Reid1, Sumithra J Mandrekar, Elsa C Carlson, W Scott Harmsen, Erin M Green, Renee M McGovern, Eva Szabo, Matthew M Ames, Daniel Boring, Paul J Limburg.   

Abstract

The cyclooxygenase (COX)-2 enzyme appears to be an important target for cancer chemoprevention. Given the recent emergence of potentially serious cardiovascular toxicity associated with selective COX-2 inhibitors, nonsteroidal antiinflammatory drugs (NSAIDs), which inhibit both COX-1 and COX-2, have received renewed attention as candidate chemoprevention agents. Sulindac has shown consistent chemopreventive potential in preclinical studies as well as in a limited number of clinical trials reported to date. For the current pharmacokinetic study, sulindac capsules were prepared to facilitate ample agent supplies for future intervention studies. Encapsulation of the parent compound (sulindac sulfoxide) can be readily accomplished, but the effects of alternate formulations on bioavailability have not been rigorously examined. In the present single-dose, two-period crossover trial, we conducted pharmacokinetic analyses of sulindac in capsule (test) versus tablet (reference) formulations. Overall, bioavailability appeared to be higher for the capsule compared with the tablet formulation based on test-to-reference pharmacokinetic variable ratios for the parent compound alone. However, additional analyses based on the sulfide and sulfone metabolites of sulindac with the same pharmacokinetic variables indicated similar chemopreventive exposures between the capsule and tablet formulations. These data support the use of sulindac capsules, which can be readily prepared with matching placebos, in future blinded chemoprevention trials.

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Year:  2008        PMID: 18349286      PMCID: PMC2435402          DOI: 10.1158/1055-9965.EPI-07-2510

Source DB:  PubMed          Journal:  Cancer Epidemiol Biomarkers Prev        ISSN: 1055-9965            Impact factor:   4.254


  25 in total

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2.  Assessment of metabolites in bioequivalence studies: should bioequivalence criteria be applied on the sum of parent compound and metabolite?

Authors:  I Mahmood
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Review 3.  Clinical pharmacokinetics of sulindac. A dynamic old drug.

Authors:  N M Davies; M S Watson
Journal:  Clin Pharmacokinet       Date:  1997-06       Impact factor: 6.447

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Authors:  C R Clark; C L McMillian; J F Hoke; K D Campagna; W R Ravis
Journal:  J Chromatogr Sci       Date:  1987-06       Impact factor: 1.618

5.  Clinical development plan: sulindac.

Authors:  G J Kelloff; J A Crowell; C W Boone; V E Steele; R A Lubet; P Greenwald; D S Alberts; J M Covey; L A Doody; G G Knapp
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Journal:  J Cell Biochem Suppl       Date:  1994

7.  Absorption of sulindac from a novel (Pro-SorbTM) liquid formulation.

Authors:  I Kanfer; C Brown; M Konings; J Swarbrick
Journal:  Biopharm Drug Dispos       Date:  1996-04       Impact factor: 1.627

8.  Sulfone metabolite of sulindac inhibits mammary carcinogenesis.

Authors:  H J Thompson; C Jiang; J Lu; R G Mehta; G A Piazza; N S Paranka; R Pamukcu; D J Ahnen
Journal:  Cancer Res       Date:  1997-01-15       Impact factor: 12.701

9.  Sulindac for polyposis of the colon.

Authors:  W R Waddell; R W Loughry
Journal:  J Surg Oncol       Date:  1983-09       Impact factor: 3.454

10.  Treatment of colonic and rectal adenomas with sulindac in familial adenomatous polyposis.

Authors:  F M Giardiello; S R Hamilton; A J Krush; S Piantadosi; L M Hylind; P Celano; S V Booker; C R Robinson; G J Offerhaus
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2.  Cytotoxic Synergy Between Cytokines and NSAIDs Associated With Idiosyncratic Hepatotoxicity Is Driven by Mitogen-Activated Protein Kinases.

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4.  Randomized phase II trial of sulindac for lung cancer chemoprevention.

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5.  Sulindac for stroke treatment: neuroprotective mechanism and therapy.

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