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Identification of novel plasma glycosylation-associated markers of aging

Authors :
Claudio Franceschi
Vincenzo Borelli
Fabio Dall'Olio
Mariella Chiricolo
Celso A. Reis
Miriam Capri
Giulia Venturi
Hugo Osório
Nadia Malagolini
Daniela Monti
Provvidenza Maria Abruzzo
Mariangela Catera
Rita Ostan
Catera, Mariangela
Borelli, Vincenzo
Malagolini, Nadia
Chiricolo, Mariella
Venturi, Giulia
Reis, Celso
Osorio, Hugo
Abruzzo, Provvidenza M.
Capri, Miriam
Monti, Daniela
Ostan, Rita
Franceschi, Claudio
Dall'Olio, Fabio
Source :
ResearcherID, Oncotarget

Abstract

The pro- or anti-inflammatory activities of immunoglobulins G (IgGs) are controlled by the structure of the glycan N-linked to Asn297 of their heavy chain. The age-associated low grade inflammation (inflammaging) is associated with increased plasmatic levels of agalactosylated IgGs terminating with N-acetylglucosamine (IgG-G0) whose biogenesis has not been fully explained. Although the biosynthesis of glycans is in general mediated by glycosyltransferases associated with internal cell membranes, the extracellular glycosylation of circulating glycoproteins mediated by plasmatic glycosyltransferases has been recently demonstrated. In this study we have investigated the relationship between plasmatic glycosyltransferases, IgG glycosylation and inflammatory and aging markers. In cohorts of individuals ranging from infancy to centenarians we determined the activity of plasmatic β4 galactosyltransferase(s) (B4GALTs) and of α2,6-sialyltransferase ST6GAL1, the glycosylation of IgG, the GlycoAge test (a glycosylation-based marker of aging) and the plasma level of inflammatory and liver damage markers. Our results show that: 1) plasmatic B4GALTs activity is a new marker of aging, showing a linear increase throughout the whole age range. 2) plasmatic ST6GAL1 was high only in children and in people above 80, showing a quadratic relationship with age. 3) Neither plasmatic glycosyltransferase correlated with markers of liver damage. 4) plasmatic ST6GAL1 showed a positive association with acute phase proteins in offspring of short lived parents, but not in centenarians or in their offspring. 5) Although the glycosylation of IgGs was not correlated with the level of the two plasmatic glycosyltransferases, it showed progressive age-associated changes consistent with a shift toward a pro-inflammatory glycotype.

Details

Database :
OpenAIRE
Journal :
ResearcherID, Oncotarget
Accession number :
edsair.doi.dedup.....2f1cff2aed9013756666d743a4ff1810