Novel ELISAs for Screening of the Biogenic Amines GABA, Glycine, β-Phenylethylamine, Agmatine, and Taurine Using One Derivatization Procedure of Whole Urine Samples

The inhibitory neurotransmitters GABA, glycine and agmatine and neuromodulators β-phenylethylamine (β-PEA) and taurine are important biogenic amines of the sympathetic and parasympathetic nervous systems in the body. Abnormalities in the metabolism of these biomarkers have been implicated in a vast...

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Veröffentlicht in:Analytical chemistry (Washington) 2010-08, Vol.82 (15), p.6526-6533
Hauptverfasser: Huisman, Han, Wynveen, Paul, Nichkova, Mikaela, Kellermann, Gottfried
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Sprache:eng
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Zusammenfassung:The inhibitory neurotransmitters GABA, glycine and agmatine and neuromodulators β-phenylethylamine (β-PEA) and taurine are important biogenic amines of the sympathetic and parasympathetic nervous systems in the body. Abnormalities in the metabolism of these biomarkers have been implicated in a vast number of neurological diseases. Novel competitive immunoassays, using one unique whole urine derivatization procedure applicable for all five biomarkers, have been developed. The determination of these biomarkers was highly reproducible: the coefficient of variance of inter- and intra-assay variation is between 3.9% and 9.8% for all assays. The assays show a good linearity in urine samples within the range of 100−400 mg Cr/dL and specificity when urine samples are spiked with biogenic amines. The recoveries are between 76 and 154%. The correlation between HPLC and ELISA for glycine and taurine (n = 10) showed regression coefficients of 0.97 and 0.98, respectively. An in vivo study on the urinary clearance of β-PEA, agmatine and taurine after oral intake by healthy individuals demonstrated the specificity and clinical significance of these new immunoassays. The immunoassays are useful for clinical and basic research where a fast and accurate assay for the screening of biogenic amines in urine is required, without preclearance of the sample.
ISSN:0003-2700
1520-6882
DOI:10.1021/ac100858u