Evidence for Earlier Stabilization of Cyclosporine Pharmacokinetics in De Novo Renal Transplant Patients Receiving a Microemulsion Formulation

Kovarik, John M.; Mueller, Edgar A.; Richard, Françoise; Niese, D.; Halloran, Philip F.; Jeffery, John; Paul, L. C.; Keown, Paul

doi:10.1097/00007890-199609270-00010

Cited by 69 publications

(26 citation statements)

References 10 publications

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“…No differences were observed when we compared CO, Cmax, C12, AUC, or Cavg obtained at day 4 or month 2, although doses were 88% higher at day 4. From month 2 to month 6, no differences were observed on dose-adjusted pharmacokinetic parameters, which suggests that pharmacokinetic stability had been achieved by month 2, as previously demonstrated by Kovarik et al [26].…”

Section: -7supporting

confidence: 76%

“…It is unlikely that the magnitude of differences observed in dose-adjusted cyclosporine pharmacokinetic parameters is exclusively due to lack of doseeconcentration linearity at cyclosporine doses used early after transplantation. Moreover, the changes in pharmacokinetics did not correlate with the increase in hemoglobin over time [26].…”

Section: -7mentioning

confidence: 85%

“…During this period, physiological and biochemical changes are greater and complicated by anesthesia and postoperative ileus, all significantly affecting the absorption of orally delivered drugs [12] and increasing the risk of acute rejection due to insufficient drug exposure [ 121. Although therapeutic cyclosporine concentrations can be achieved more rapidly and with lower doses of cyclosporine microemulsion than with the oil-based formulation [l], the higher initial cyclosporine doses necessary during this period complicate cyclosporine dose adjustment, because these doses lie outside the linear doseconcentration range [26,381. Alternatively, pre-transplant cyclosporine test doses, which could minimize this difficulty, have failed to predict consistently and accurately initial doses in the majority of patients and are very difficult to determine, especially in recipients of cadaveric allografts [7].…”

Section: Introductionmentioning

confidence: 99%

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Time-dependent changes in cyclosporine exposure: implications for achieving target concentrations

et al. 2003

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This study analyzed early changes in trough blood cyclosporine concentrations and cyclosporine exposures after kidney transplantation. Seventy-two patients who received cyclosporine-based immunosuppressive therapy were intensively monitored (CO) during the first 6 months after transplantation. Full pharmacokinetic studies were performed at day 4, and months 2, 3, and 6 after transplantation. Mean steady-state, dose-adjusted trough cyclosporine blood concentrations increased from 1.1 f 0.60 (day 7) to 2.0 i 1.20 ng/ml per mg (day 30, P < 0.01). Steadystate, dose-adjusted cyclosporine exposure parameters (CO, Cmax, AUC, Cavg, and Cl2) were significantly lower at day 4 than at months 2, 3, and 6 after transplantation (P < 0.01). Initial cyclosporine doses produced target concentrations in only 30% of the patients at day 3. C2 was the single concentration that showed high and consistent correlation with serial AUC measurements (y2 2 0.76). The incidence of biopsy-proven acute rejection was 20.5% and was not associated with ethnicity, HLA mismatch, adjunctive therapy, or blood trough cyclosporine concentrations below 200 ng/ml at day 3. Significant time-dependent increases in steadystate cyclosporine exposure occur during the first month after kidney transplantation. Due to the low relative bioavailability early after surgery, higher doses and more frequent cyclosporine dose adjustments are necessary to produce target exposures early after transplantation.

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Section: -7supporting

confidence: 76%

Section: -7mentioning

confidence: 85%

Section: Introductionmentioning

confidence: 99%

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Time-dependent changes in cyclosporine exposure: implications for achieving target concentrations

et al. 2003

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“…Patient 6 was in remission during both pharmacokinetic profiles, and is the only one in whom the AUC was higher at 24 weeks. A higher CsA bioavailability over time has been reported in transplant recipients [37,38] and has been attributed to increased cyclosporine binding to blood components (rise in hematocrit), rather than changes in metabolism or elimination. In our study, the difference in hematocrit between 1 and 24 weeks was not statistically significant.…”

Section: Discussionmentioning

confidence: 97%

Decreased cyclosporine exposure during the remission of nephrotic syndrome

et al. 2007

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In this paper, we report the pharmacokinetics changes observed in seven children with steroid-resistant nephrotic syndrome (SRNS). They received cyclosporine A (CsA) microemulsion 6 mg/kg/day and, one week later, they were admitted to perform a 12-h pharmacokinetic profile with eight time sample points. The pharmacokinetic profile was repeated at 24 weeks of treatment, when all patients achieved remission. Blood concentration against time curves were constructed for each patient at weeks 1 and 24 of CsA treatment. Peak concentrations (C (max)) and the time needed to reach peak concentrations (t (max)) were directly determined from these plots. The area under the curve (AUC) was estimated by the trapezoidal rule. There was a statistically significant difference of the AUC, trough levels, and t (max) between weeks 1 and 24, with a decrease of AUC from 5,211 ng*h/ml in week 1 to 3,289 ng*h/ml in week 24, the trough levels decreased from 157 ng/ml to 96 ng/ml, and the t (max) decreased from 1.85 h to 1.00 h. The higher CsA bioavailability during the nephrotic state has to be considered when managing patients, since the target AUC cannot be the same throughout the treatment.

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“…CsA microemulsion has been accepted as a superior vehicle for oral administration and produces more linear, rapid, constant and complete absorption of CsA than previous formulations. 7,8 Microemulsion decreases both interpatient and intrapatient variability of CsA levels, 9,10 resulting in more predictable pharmacokinetics. 11 Tacrolimus (FK506).…”

Section: Calcineurin Inhibitors (Csa and Tacrolimus)mentioning

confidence: 99%

Immunosuppressive agents in transplantation: Mechanisms of action and current anti-rejection strategies

et al. 2000

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Evidence for Earlier Stabilization of Cyclosporine Pharmacokinetics in De Novo Renal Transplant Patients Receiving a Microemulsion Formulation

Cited by 69 publications

References 10 publications

Time-dependent changes in cyclosporine exposure: implications for achieving target concentrations

Time-dependent changes in cyclosporine exposure: implications for achieving target concentrations

Decreased cyclosporine exposure during the remission of nephrotic syndrome

Immunosuppressive agents in transplantation: Mechanisms of action and current anti-rejection strategies

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