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The Cerebrospinal Fluid Free-Glycans Hexsub.1 and HexNAcsub.1Hexsub.1Neu5Acsub.1 as Potential Biomarkers of Alzheimer’s Disease
The Cerebrospinal Fluid Free-Glycans Hexsub.1 and HexNAcsub.1Hexsub.1Neu5Acsub.1 as Potential Biomarkers of Alzheimer’s Disease
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The Cerebrospinal Fluid Free-Glycans Hexsub.1 and HexNAcsub.1Hexsub.1Neu5Acsub.1 as Potential Biomarkers of Alzheimer’s Disease
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The Cerebrospinal Fluid Free-Glycans Hexsub.1 and HexNAcsub.1Hexsub.1Neu5Acsub.1 as Potential Biomarkers of Alzheimer’s Disease
The Cerebrospinal Fluid Free-Glycans Hexsub.1 and HexNAcsub.1Hexsub.1Neu5Acsub.1 as Potential Biomarkers of Alzheimer’s Disease

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The Cerebrospinal Fluid Free-Glycans Hexsub.1 and HexNAcsub.1Hexsub.1Neu5Acsub.1 as Potential Biomarkers of Alzheimer’s Disease
The Cerebrospinal Fluid Free-Glycans Hexsub.1 and HexNAcsub.1Hexsub.1Neu5Acsub.1 as Potential Biomarkers of Alzheimer’s Disease
Journal Article

The Cerebrospinal Fluid Free-Glycans Hexsub.1 and HexNAcsub.1Hexsub.1Neu5Acsub.1 as Potential Biomarkers of Alzheimer’s Disease

2024
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Overview
Alzheimer’s disease (AD) is the most common neurodegenerative disorder, affecting a growing number of elderly people. In order to improve the early and differential diagnosis of AD, better biomarkers are needed. Glycosylation is a protein post-translational modification that is modulated in the course of many diseases, including neurodegeneration. Aiming to improve AD diagnosis and differential diagnosis through glycan analytics methods, we report the glycoprotein glycome of cerebrospinal fluid (CSF) isolated from a total study cohort of 262 subjects. The study cohort consisted of patients with AD, healthy controls and patients suffering from other types of dementia. CSF free-glycans were also isolated and analyzed in this study, and the results reported for the first time the presence of 19 free glycans in this body fluid. The free-glycans consisted of complete or truncated N-/O-glycans as well as free monosaccharides. The free-glycans Hex[sub.1] and HexNAc[sub.1] Hex[sub.1] Neu5Ac[sub.1] were able to discriminate AD from controls and from patients suffering from other types of dementia. Regarding CSF N-glycosylation, high proportions of high-mannose, biantennary bisecting core-fucosylated N-glycans were found, whereby only about 20% of the N-glycans were sialylated. O-Glycans and free-glycan fragments were less sialylated in AD patients than in controls. To conclude, this comprehensive study revealed for the first time the biomarker potential of free glycans for the differential diagnosis of AD.

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