Estimation of individual sensitivity to cyclosporin in children awaiting renal transplantation

doi:10.1093/ndt/18.2.403

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Nephrol Dial Transplant (2003) 18: 403-410
© 2003 European Renal Association-European Dialysis and Transplant Association

Estimation of individual sensitivity to cyclosporin in children awaiting renal transplantation

Jan Dudley¹^,2^,, Carol Truman¹, Mary McGraw², Jane Tizard², Gausal Haque¹ and Ben Bradley¹

¹ University of Bristol Department of Transplantation Sciences and ² Department of Paediatric Nephrology, Bristol Royal Hospital for Children, Bristol, UK

Background. Optimal immunosuppressive drug therapy requiresthat efficacy be balanced against toxicity. We have performedin vitro assays of cyclosporin (CsA) efficacy in children awaitingrenal transplantation.

Methods. Peripheral blood mononuclear cells (PBMC) from13 children awaiting renal transplantation and 10 healthy paediatriccontrols (‘responders’) were incubated in the presenceof CsA (0–250 ng/ml). Irradiated PBMC from a parent (prospectivelive donor) were cultured with those of the child in the presenceof interleukin 2. Europium-labelled, non-irradiated phytohaemagluttinin-stimulatedtarget cells from the parent were added to the culture after7 days incubation. Target cell lysis was quantified by timeresolved fluorometry. CsA-mediated inhibition of target celllysis was calculated and used to compare individual responsesto the drug. Two-colour flow cytometry was performed to identifyactivated subsets of lymphocytes at varying concentrations ofCsA.

Results. Wide inter-individual variations in per cent lysisand per cent inhibition were observed in patients and controls.Immunophenotyping indicated expansion of CD8⁺ and CD25⁺ lymphocytesubsets following allo-stimulation that was inhibited by increasingconcentrations of CsA. Eight out of 13 patients and four outof 10 controls were ‘sensitive’ to CsA in vitroin that they achieved 50% inhibition of cell lysis (IC₅₀) atlow concentrations of the drug (<50 ng/ml). Eleven patientshave subsequently received a renal transplant. Five out of sevenof these patients with IC₅₀ <50 ng/ml have suffered problemswith infection, nephrotoxicity and graft vasculopathy raisingthe possibility of ‘over-immunosuppression’.

Conclusion. The data imply a useful role for this modelin the prediction of individual response to immunosuppressionfollowing allo-stimulation in the pre-transplant setting.

Keywords: allo-specificity; cyclosporin; cytotoxic T lymphocyte; renal transplantation

Correspondence and offprint requests to: Dr J. Dudley, Universityof Bristol Department of Transplantation Sciences, Paul O'GormanLifeline Centre, Southmead Hospital, Bristol BS10 5NB, UK. Email:jandudley{at}yahoo.com

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Nephrology Dialysis Transplantation

Estimation of individual sensitivity to cyclosporin in children awaiting renal transplantation