Publication | Closed Access
Clinical evaluation of 5-S-cysteinyldopa testing using a new and optimized detection system as a tumour marker for malignant melanoma
10
Citations
26
References
2002
Year
EngineeringDiagnosisPathologyMalignant MelanomaDermatologyTumor BiologyCancer DetectionBioanalysisIv Malignant MelanomaAnalytical ChemistryMelanoma PatientsBiomarker DiscoveryClinical ChemistryLiquid ChromatographyLaboratory MedicineMolecular DiagnosticsClinical EvaluationMolecular ImagingCancer ResearchChromatographyRadiologySolid Phase ExtractionSkin CancerMedicineMelanomaTumor MicroenvironmentTumour MarkerInnovative DiagnosticsOncology
5-S-cysteinyldopa (5-S-CD) has been described as a tumour marker for the detection of human metastatic melanoma. We investigated the clinical utility of a new and optimized method to detect 5-S-CD by analysing 207 plasma samples derived from 138 patients with clinical stage I/II ( = 60), III ( = 32) or IV ( = 46) melanoma. Control groups consisted of 27 patients with non-melanoma skin diseases and 30 healthy volunteers. 5-S-CD plasma levels were determined using a new analytical technique based on a fully automated solid phase extraction coupled online to a novel high performance liquid chromatography method. In all the samples from the healthy control subjects 5-S-CD plasma concentrations were below 2.0 microg/l. Increased 5-S-CD-levels (>/=2.0 microg/l) were found in 52%, 67% and 81% of the plasma samples from patients with stages I/II, III and IV malignant melanoma, respectively. The mean values of 5-S-CD were found to rise with increasing tumour stage. Among 27 samples from patients with non-melanoma skin disease, slightly elevated 5-S-CD levels between 2.3 and 2.6 microg/l were found in only four samples from patients with multiple dysplastic naevi. In conclusion, our improved analytical technique provides a high sensitivity in all stages of the disease and represents a useful technique for monitoring melanoma patients.
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