Pharmacogenetics of immunosuppressive drugs: prospect of individual therapy for transplant patients

Author:

Ekbal Nasirul J1,Holt David W2,MacPhee Iain AM1

Affiliation:

1. St George’s, University of London, Cellular and Molecular Medicine: Renal Medicine, Cranmer Terrace, London, SW17 0RE, UK.

2. St George’s, University of London, Cardiac and Vascular Sciences: Analytical Unit, Cranmer Terrace, London, SW17 0RE, UK

Abstract

The immunosuppressive drugs used in solid-organ transplantation are potent and toxic agents with narrow therapeutic ranges. Underdosing is associated with immunological rejection of the transplanted organ, whereas overdosing results in infections, malignancy and direct toxicity to a number of organs. Pharmacokinetic heterogeneity makes initial dose determination difficult, as there is a poor correlation between dose and blood concentration. Therapeutic drug monitoring is available but the pharmacokinetic–pharmacodynamic association is imperfect and it does not help in achieving target blood concentrations during the critical early 2–3 days after transplantation. Genetic polymorphisms in drug targets, drug-metabolizing enzymes and drug efflux pumps have been identified as potential targets for developing a pharmacogenetic strategy to individualize initial drug choice and dose. To date, use of the CYP3A5 genotype to predict the appropriate initial dose of tacrolimus is the most promising option for individualization of drug therapy in organ transplantation.

Publisher

Future Medicine Ltd

Subject

Pharmacology,Genetics,Molecular Medicine

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