Elsa C. Carlson scite author profile

Elsa C. Carlson

5Publications

30Citation Statements Received

95Citation Statements Given

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Affiliations

Mayo Clinic, Winneshiek Medical Center

Publications

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Comparative Bioavailability of Sulindac in Capsule and Tablet Formulations

Reid¹,

Mandrekar²,

Carlson

et al. 2008

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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 singledose, 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. (Cancer Epidemiol Biomarkers Prev 2008;17(3):674 -9)

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Population Pharmacokinetic Model for Cancer Chemoprevention With Sulindac in Healthy Subjects

Berg

Mandrekar

Ziegler

et al. 2013

The Journal of Clinical Pharma

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Sulindac is a prescription-based non-steroidal anti-inflammatory drug (NSAID) that continues to be actively investigated as a candidate cancer chemoprevention agent. To further current understanding of sulindac bioavailability, metabolism, and disposition, we developed a population pharmacokinetic model for the parent compound and its active metabolites, sulindac sulfide, and exisulind. This analysis was based on data from 24 healthy subjects who participated in a bioequivalence study comparing two formulations of sulindac. The complex disposition of sulindac and its metabolites was described by a seven-compartment model featuring enterohepatic recirculation and is the first reported population pharmacokinetic model for sulindac. The derived model was used to explore effects of clinical variables on sulindac pharmacokinetics and revealed that body weight, creatinine clearance, and gender were significantly correlated with pharmacokinetic parameters. Moreover, the model quantifies the relative bioavailability of the sulindac formulations and illustrates the utility of population pharmacokinetics in bioequivalence assessment. This novel population pharmacokinetic model provides new insights regarding the factors that may affect the pharmacokinetics of sulindac and the exisulind and sulindac sulfide metabolites in generally healthy subjects, which have implications for future chemoprevention trial design for this widely available agent.

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High compliance can be achieved in an adenoma prevention clinical trial

Larson¹,

Carlson²

2000

Gastroenterology

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Prevalence of ileal neoplasms and colonic metaplasia in familial adenomatous polyposis patients after proctocolectomy: A prospective study

Geller¹,

Smyrk²,

Carlson³

et al. 2001

Gastroenterology

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A computerized colorectal cancer prevention registry and risk assessment tool

Timmons¹,

Carlson²,

King³

et al. 1998

Gastroenterology

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Elsa C. Carlson

Comparative Bioavailability of Sulindac in Capsule and Tablet Formulations

Population Pharmacokinetic Model for Cancer Chemoprevention With Sulindac in Healthy Subjects

High compliance can be achieved in an adenoma prevention clinical trial

Prevalence of ileal neoplasms and colonic metaplasia in familial adenomatous polyposis patients after proctocolectomy: A prospective study

A computerized colorectal cancer prevention registry and risk assessment tool

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