Sandimmune®to neoral®conversion and value of abbreviated AUC monitoring in stable pediatric kidney transplant recipients

Abstract

Neoral^®is a new microemulsion formulation of cyclosporin A (CsA) that has been reported to have better absorption characteristics than sandimmune^®. We converted 25 long‐term pediatric renal transplant recipients with a mean age of 14.1 yr and a mean follow‐up period of 6.4 yr from sandimmune (SIM) to neoral (NEO) on a 1 : 1 basis. The mean dosage of SIM or NEO required to maintain ‘therapeutic range’ steady‐state trough levels between 100 and 200 ng/mL was similar. We compared 6‐h CsA pharmacokinetic profiles taken approximately 6 months after the conversion to NEO with the previous SIM profiles of the same patients. Generally, in the NEO profiles the time to reach the maximum concentration was shorter and the maximum concentration was higher, showing a rapid decline towards the trough‐level when compared to the previous SIM profiles. During intake of NEO the AUC_0–12 hin the 12‐h profiles correlates strongly with the AUC_0–6 hin the 6‐h profiles (r = 0.98), a similar finding to that which we reported previously for SIM. The median AUC_0–6 hfor NEO demonstrates a 70% increase compared to the median AUC_0–6 hfor SIM. Despite the increased drug exposure NEO was well tolerated and did not cause any apparent toxicity within the first 6 months after conversion. The CsA blood level 2 h after intake of NEO showed a higher correlation with the AUC_0–12 h(r = 0.91) than the trough level (r = 0.64). The abbreviated profile based on three early sampling points and calculated by AUC_PRED= 335.9 + 1.1*(C₁) + 1.1*(C₂) + 5.4*(C₄) correlated well with the full AUC (r² = 0.98, p < 0.0001). Mean prediction error (±SD) was 0.16% (±4.32), and in no patients did the calculated values fall outside the 10% prediction error limit. We therefore conclude that NEO exhibits a higher bioavailability in children compared to SIM without causing apparent toxicity. Monitoring of the C₂might be a better alternative for trough level monitoring in daily clinical practice. A strategy of three early sampling points (C₁, C₂and C₄) allows a reliable AUC_0–12 hprediction and can reduce the length of observation, making it a useful and cost‐effective tool in clinical practice.