Clinical Pharmacokinetics of Pregabalin in Healthy Volunteers
Corresponding Author
Dr Howard N. Bockbrader PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Address for correspondence: Howard N. Bockbrader, PhD, Pfizer Global Research & Development, 50 Pequot Ave, New London, CT 06320; e-mail: [email protected].Search for more papers by this authorDr Louis L. Radulovic PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Fulcrum Pharma Developments, Inc, Ann Arbor, Michigan
Search for more papers by this authorDr Edward L. Posvar MD, MPH
From Pfizer Global Research & Development, Ann Arbor, Michigan
Amgen Inc, Thousand Oaks, California
Search for more papers by this authorDr James C. Strand PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Search for more papers by this authorDr Christine W. Alvey BS
From Pfizer Global Research & Development, Ann Arbor, Michigan
Search for more papers by this authorDr Janice A. Busch BS
From Pfizer Global Research & Development, Ann Arbor, Michigan
Search for more papers by this authorDr Edward J. Randinitis PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Search for more papers by this authorDr Brian W. Corrigan PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Search for more papers by this authorDr George M. Haig PharmD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Abbott Laboratories, Chicago, Illinois
Search for more papers by this authorDr Rebecca A. Boyd PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Search for more papers by this authorDr David L. Wesche MD, PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
MMS Holdings, Canton, Michigan.
Search for more papers by this authorCorresponding Author
Dr Howard N. Bockbrader PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Address for correspondence: Howard N. Bockbrader, PhD, Pfizer Global Research & Development, 50 Pequot Ave, New London, CT 06320; e-mail: [email protected].Search for more papers by this authorDr Louis L. Radulovic PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Fulcrum Pharma Developments, Inc, Ann Arbor, Michigan
Search for more papers by this authorDr Edward L. Posvar MD, MPH
From Pfizer Global Research & Development, Ann Arbor, Michigan
Amgen Inc, Thousand Oaks, California
Search for more papers by this authorDr James C. Strand PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Search for more papers by this authorDr Christine W. Alvey BS
From Pfizer Global Research & Development, Ann Arbor, Michigan
Search for more papers by this authorDr Janice A. Busch BS
From Pfizer Global Research & Development, Ann Arbor, Michigan
Search for more papers by this authorDr Edward J. Randinitis PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Search for more papers by this authorDr Brian W. Corrigan PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Search for more papers by this authorDr George M. Haig PharmD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Abbott Laboratories, Chicago, Illinois
Search for more papers by this authorDr Rebecca A. Boyd PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
Search for more papers by this authorDr David L. Wesche MD, PhD
From Pfizer Global Research & Development, Ann Arbor, Michigan
MMS Holdings, Canton, Michigan.
Search for more papers by this authorAbstract
Pregabalin has shown clinical efficacy for treatment of neuropathic pain syndromes, partial seizures, and anxiety disorders. Five studies in healthy volunteers are performed to investigate single- and multiple-dose pharmacokinetics of pregabalin. Pregabalin is rapidly absorbed following oral administration, with peak plasma concentrations occurring between 0.7 and 1.3 hours. Pregabalin oral bioavailability is approximately 90% and is independent of dose and frequency of administration. Food reduces the rate of pregabalin absorption, resulting in lower and delayed maximum plasma concentrations, yet the extent of drug absorption is unaffected, suggesting that pregabalin may be administered without regard to meals. Pregabalin elimination half-life is approximately 6 hours and steady state is achieved within 1 to 2 days of repeated administration. Corrected for oral bioavailability, pregabalin plasma clearance is essentially equivalent to renal clearance, indicating that pregabalin undergoes negligible nonrenal elimination. Pregabalin demonstrates desirable, predictable pharmacokinetic properties that suggest ease of use. Because pregabalin is eliminated renally, renal function affects its pharmacokinetics.
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