Urine acylcarnitine analysis by ESI-MS/MS: a new tool for the diagnosis of peroxisomal biogenesis disorders.

[zellweger syndrome]

Patients with peroxisomal biogenesis disorders (PBDs ) have an abnormal profile of circulating acylcarnitines (i .e . elevated C 16 :0 -DC -, C 18 :0 -DC -, C 2 4 :0 -, C 2 6 :0 -carnitine ). We developed an ESI -MS /MS method for quantification of urine acylcarnitines and tested its reliability for the diagnosis of PBDs .U rine from 7 patients with PBDs (5 Zellweger syndrome , 2 infantile Refsum disease ), from 2 patients with D-bifunctional protein (D-BP ) deficiency , and from 130 healthy controls were analysed by ESI -MS /MS , using a multiple reactions monitoring (MRM ) method , and quantified with labelled internal standards . Acylcarnitine levels between groups were analyzed by the STATA statistics data analysis and compared by the non parametric Mann-Whitney test .In PBDs , the urinary excretion of long -chain dicarboxylylcarnitines (C 14 :0 -DC -, C 16 :0 -DC -, and C 18 :0 -DC -carnitine ), and of very long -chain monocarboxylylcarnitines (C 2 2 :0 -, C 2 4 :0 -, C 2 6 :0 -carnitine ) were significantly elevated compared to controls (p <0 .0001 ). Interestingly , among PBDs the most severe abnormalities of acylcarnitine profile were observed in patients with Zellweger syndrome . One patient with D-BP showed similar abnormalities to PBDs , while in the other only C 16 :0 -DC -carnitine was markedly elevated .This study shows that MRM ESI -MS /MS acylcarnitine analysis unequivocally discriminates patients with PBDs and D-BP deficiency from controls , representing a reliable and sensitive method for the diagnosis that requires a short -time analysis with high sample through-put .