MRP2 encoded by ABCC2 gene is involved in the secretion of numerous drugs and endogenous substrates. Patients with Dubin-Johnson syndrome due to mutation in ABCC2 gene have elevated urinary coproporphyrin ratio (UCP I/(I + III)). Here we investigated whether this ratio could serve as a biomarker of MRP2 function. Phenotype-genotype relationships were studied in 74 healthy subjects by measuring individual UCP I/(I + III) ratio obtained on 24-hour urine and by analyzing five common SNPs in ABCC2 gene. The UCP I/(I + III) ratio varied from 14.7 to 46.0 in our population. Subjects with 3972TT genotype had a higher ratio (P =.04) than those carrying the C allele. This higher UCP I/(I + III) ratio was correlated with a higher level of isomer I excretion. This study provides a proof of concept that UCP I/(I + III) ratio can be used as a biomarker of MRP2 function in clinical studies as it provides quantitative information about the in vivo activity of MRP2 in a given patient. Copyright 2011 Isabelle Benz-de Bretagne et al.
CITATION STYLE
Le Guellec, C., Benz-De Bretagne, I., Respaud, R., Vourc’H, P., Halimi, J. M., Caille, A., … Andres, C. R. (2011). Urinary elimination of coproporphyrins is dependent on ABCC2 polymorphisms and represents a potential biomarker of MRP2 activity in humans. Journal of Biomedicine and Biotechnology, 2011. https://doi.org/10.1155/2011/498757
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