Differentiation of innovator versus generic cyclosporine via a drug interaction on sirolimus

Both sirolimus and cyclosporine are immunosuppressants used in a combined regimen after organ transplantation. When coadministered with the innovator formulation of cyclosporine, sirolimus blood levels increase 3.3-fold due to a pharmacokinetic interaction. We assessed this drug interaction for pote...

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Bibliographic Details
Published in:European journal of clinical pharmacology 2006-05, Vol.62 (5), p.361-366
Main Authors: KOVARIK, John M, NOE, Adele, YIBIN WANG, MUELLER, Irene, DENUCCI, Gilberto, SCHMOUDER, Robert L
Format: Article
Language:English
Subjects:
Adult
Aged
Analysis of Variance
Animals
Area Under Curve
Biological and medical sciences
Chemistry, Pharmaceutical
Cross-Over Studies
Cyclosporine - administration & dosage
Cyclosporine - pharmacokinetics
Dogs
Drug Interactions
Drug Prescriptions
Drug Therapy, Combination
Drugs, Generic
Fasting
Female
Humans
Immunosuppressive Agents - administration & dosage
Immunosuppressive Agents - pharmacokinetics
Kidney Transplantation
Male
Medical sciences
Middle Aged
Pharmacology. Drug treatments
Sirolimus - administration & dosage
Sirolimus - pharmacokinetics
Therapeutic Equivalency
Time Factors
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Summary:Both sirolimus and cyclosporine are immunosuppressants used in a combined regimen after organ transplantation. When coadministered with the innovator formulation of cyclosporine, sirolimus blood levels increase 3.3-fold due to a pharmacokinetic interaction. We assessed this drug interaction for potential differences when the innovator formulation is replaced by a generic cyclosporine. In this randomized single-dose crossover study, 28 healthy subjects received 5 mg sirolimus oral solution with 250 mg cyclosporine soft gelatin capsules given as the innovator formulation (reference treatment) versus a generic formulation (test treatment). Sirolimus peak blood concentration (Cmax) and area under the concentration-time curve (AUC) were compared between test and reference treatments by standard bioequivalence testing. Sirolimus Cmax was significantly lower by 17% in the presence of generic versus innovator cyclosporine (p=0.0003) and failed bioequivalence criteria with a test/reference ratio of 0.83 (90% confidence interval, 0.77-0.90). Nearly half of the subjects (46%) had sirolimus Cmax changes which fell outside the bioequivalence window with individual Cmax decreases up to 52% and increases up to 39%. Sirolimus AUC was significantly lower by 11% in the presence of generic versus innovator cyclosporine (p=0.041) but satisfied average bioequivalence criteria with a test/reference ratio of 0.89 (0.83-0.95). Nonetheless, over a third of the subjects (43%) had sirolimus AUC changes outside the standard bioequivalence window with individual AUC decreases up to 39% and increases up to 42%. Switching between innovator and generic cyclosporine may have a clinically-relevant impact on coadministered sirolimus pharmacokinetics. If such a switch is initiated by the prescriber, follow-up therapeutic monitoring of both cyclosporine and sirolimus blood levels should be performed to guide dose adjustments as necessary. If the switch is made without consulting the prescriber, potentially significant changes in sirolimus exposure could go unnoticed by the clinician and patient.
ISSN:0031-6970
1432-1041
DOI:10.1007/s00228-006-0109-z