| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 8633048 | Metabolism | 2018 | 7 Pages |
Abstract
Due to a lack of an enzymatic assay for GSD type III and a certain unreliability of the assay for GSD type IX, our finding could help clinicians in differential diagnosis to better target and select appropriate genetic analysis for the suspected patients. We hypothesize that the detected profound ApoC-III hypoglycosylation in these two disorders results from reduced availability of the nucleotide-monosaccharides, specifically UDP-GalNAc, in the corresponding glycosylation reactions.
Keywords
TransferrinUDP-GalNacN-acetylgalactosamineGalNAcTHRNeuAcCDGApoC-IIIUDP-GlcUDP-GalGSDO-GlycosylationCMP-NeuAcGlc-1-Puridine diphosphate galactoseApolipoprotein C-IIICongenital disorders of glycosylationthreonineTriacylglycerolsTAG یا triacylglycerols Diagnostic markerHypertriglyceridemiaCHECholinesteraseGalGalactoseglucose-1-phosphateuridine diphosphate glucose
Related Topics
Life Sciences
Biochemistry, Genetics and Molecular Biology
Endocrinology
Authors
Nina Ondruskova, Tomas Honzik, Hana Kolarova, Zuzana Pakanova, Jan Mucha, Jiri Zeman, Hana Hansikova,