Your search keyword '"Gudelj, Ivan"' showing total 6 results

1. IgG N-Glycosylation Is Altered in Coronary Artery Disease.

Author

Radovani, Barbara, Vučković, Frano, Maggioni, Aldo P., Ferrannini, Ele, Lauc, Gordan, and Gudelj, Ivan

Subjects

CORONARY artery disease, IMMUNOGLOBULIN G, POST-translational modification, HYDROPHILIC interaction liquid chromatography, IMMUNE response, FC receptors

Abstract

Coronary artery disease (CAD) is the most common cardiovascular disease (CVD), and previous studies have shown a significant association between N-glycosylation, a highly regulated posttranslational modification, and the development of atherosclerotic plaques. Our aim was to determine whether the N-glycome of immunoglobulin G (IgG) is associated with CAD, as N-glycans are known to alter the effector functions of IgG, which may enhance the inflammatory response in CAD. Therefore, in this study, we isolated IgG from subjects with coronary atherosclerosis (CAD+) and from subjects with clean coronaries (CAD−). The purified IgGs were denatured and enzymatically deglycosylated, and the released and fluorescently labelled N-glycans were analysed by ultra-high performance liquid chromatography based on hydrophilic interactions with fluorescence detection (HILIC-UHPLC-FLR). Sex-stratified analysis of 316 CAD− and 156 CAD+ cases revealed differences in IgG N-glycome composition. The most notable differences were observed in women, where the presence of sialylated N-glycan structures was negatively associated with CAD. The obtained chromatograms provide insight into the IgG N-glycome composition in CAD as well as the biomarker potential of IgG N-glycans in CAD. [ABSTRACT FROM AUTHOR]

Published

2023

2. N-Glycosylation and Inflammation; the Not-So-Sweet Relation.

Author

Radovani, Barbara and Gudelj, Ivan

Subjects

IMMUNE response, NATURAL immunity, INFLAMMATION, CELLULAR signal transduction, GLYCOSYLTRANSFERASES

Abstract

Chronic inflammation is the main feature of many long-term inflammatory diseases such as autoimmune diseases, metabolic disorders, and cancer. There is a growing number of studies in which alterations of N-glycosylation have been observed in many pathophysiological conditions, yet studies of the underlying mechanisms that precede N-glycome changes are still sparse. Proinflammatory cytokines have been shown to alter the substrate synthesis pathways as well as the expression of glycosyltransferases required for the biosynthesis of N-glycans. The resulting N-glycosylation changes can further contribute to disease pathogenesis through modulation of various aspects of immune cell processes, including those relevant to pathogen recognition and fine-tuning the inflammatory response. This review summarizes our current knowledge of inflammation-induced N-glycosylation changes, with a particular focus on specific subsets of immune cells of innate and adaptive immunity and how these changes affect their effector functions, cell interactions, and signal transduction. [ABSTRACT FROM AUTHOR]

Published

2022

3. Spatio-temporal profiling of the human brain N- glycome

Author

Klarić, Thomas, Gudelj, Ivan, Vučković, Frano, Novokmet, Mislav, Bečeheli, Ivona, Šestan, Nenad, and Lauc, Gordan

Subjects

carbohydrates (lipids), Neuroglycobiology, N-glycome, N-glycans

Abstract

N-glycosylation plays a role in many aspects of nervous system biology including membrane excitability, synaptic transmission, maintenance and differentiation of neural stem cells, neurite outgrowth and neuronal plasticity [1–6]. Yet there are remarkably few studies that have attempted to characterize the N-glycome of the brain in detail [7-10]. An in-depth structural characterization of the neuroglycome is therefore of great importance to gain a better understanding of glycan functions in the central nervous system. The goal of the project was to characterise the spatiotemporal profile of N-glycan structures in the human brain and how they change throughout ontogeny. To achieve this, a new method was developed to allow rapid analysis of N-glycans from brain tissue by HILIC-UPLC. Structural annotation of N-glycans was performed by MALDI-TOF/TOF MS/MS. The main finding from this work is that evolutionarily older brain regions, such as the cerebellum and striatum, tend to contain simpler N-glycans, including a large proportion of oligomannose structures, while more recently evolved brain regions, such as the hippocampus and frontal cortex, tend to have more complex N-glycans, including highly branched, tri- and tetra-antennary structures. Similarly, a shift in the brain N-glycome profile is observed during development with simpler N-glycans, particularly oligomannose structures, being common in the fetal brain, but more complex structures being prevalent in the adult brain. These findings lead us to hypothesize that there is an association between the complexity of N-glycan structures in a given brain region and the level of functional complexity.

Published

2017

4. Biomarker Potential of Plasma Protein N-glycans in Coronary Artery Disease.

Author

Blivajs, Aleksandar, Radovani, Barbara, Đerek, Lovorka, Rudan, Diana, Visentin, David, Lauc, Gordan, and Gudelj, Ivan

Subjects

ATHEROSCLEROTIC plaque, BLOOD proteins, CORONARY artery disease, PLASMA potentials, HYDROPHILIC interaction liquid chromatography, STRESS echocardiography, ARTERITIS, AFFINITY chromatography

Abstract

Introduction: Coronary artery disease (CAD) is the most common cardiovascular disease (CVD), resulting from chronic inflammation of the coronary arteries due to the formation of atherosclerotic plaques, and its presence is a significant marker of adverse cardiovascular events. A growing body of research suggests that alterations in protein N-glycosylation are involved in the development of CVD through various mechanisms and have significant biomarker potential because of their sensitivity to changes that occur in the organism during inflammation-related conditions such as CVD1-3. Our aim was to determine whether the N-glycome of total plasma proteins is associated with CAD, because Nglycans are known to alter the effector functions of proteins, which may enhance their inflammatory response in CAD. Patients and Methods: In this study, we analysed the N-glycome of plasma proteins isolated from patients who underwent coronary angiography and classified into patients with confirmed coronary atherosclerosis and patients with clean coronaries. Proteins were denatured and enzymatically deglycosylated, and the released and fluorescently labelled N-glycans were analysed by ultra-high performance liquid chromatography based on hydrophilic interactions with fluorescence detection (HILIC-UHPLC-FLR) (Figure 1). Because previous studies have shown evidence of sexual dimorphism in CVD and significant sex differences in the association of N-glycans with CVD risk, we performed sex-stratified analysis of plasma N-glycans. Results: The results showed significant differences in plasma N-glycome composition in CAD. Lower abundance of complex biantennary galactosylated N-glycans with core fucose and, conversely, a higher abundance of highly branched (tri- and tetra-antennary) sialylated N-glycan structures with terminal fucose was shown to be associated with CAD. Conclusion: The obtained chromatograms shed light on the composition of plasma protein N-glycans in CAD and provided new insights into N-glycosylation changes in CAD. Overall, because of their sensitivity to changes that occur in an organism, protein Nglycosylation emerges as a significant factor in CAD and holds potential as a diagnostic tool, with glycan-based biomarkers showing promise for predicting cardiovascular health. [ABSTRACT FROM AUTHOR]

Published

2023

5. Low galactosylation of IgG associates with higher risk for future diagnosis of rheumatoid arthritis during 10 years of follow-up.

Author

Gudelj, Ivan, Salo, Perttu P., Trbojević-Akmačić, Irena, Albers, Malena, Primorac, Dragan, Perola, Markus, and Lauc, Gordan

Subjects

*IMMUNOGLOBULIN G, *RHEUMATOID arthritis, *AUTOANTIBODIES, *GLYCOSYLATION, *HYDROPHILIC interactions, *PATIENTS

Abstract

Antibodies are known to have an important role in the development of rheumatoid arthritis (RA), one of the most prevalent chronic inflammatory diseases which primarily involves the joints. Most RA patients develop autoantibodies against immunoglobulin G (IgG) and changes in IgG glycosylation have been associated with RA. We undertook this study to determine whether altered IgG glycosylation precedes the disease diagnosis. We studied IgG glycosylation in RA in two prospective cohorts ( N  = 14,749) by measuring 28 IgG glycan traits in 179 subjects who developed RA within 10-years follow-up and 358 matched controls. Ultra-performance liquid chromatography method based on hydrophilic interactions (HILIC-UPLC) was used to analyse IgG glycans. Future RA diagnosis associated with traits related to lower galactosylation and sialylation of IgG when comparing the cases to the matched controls. In RA cases, these traits did not correlate with the time between being recruited to the study and being diagnosed with RA (median time 4.31 years). The difference in IgG glycosylation was relatively stable and present years before diagnosis. This indicates that long-acting factors affecting IgG glycome composition are among the underlying mechanisms of RA and that decreased galactosylation is a pre-existing risk factor involved in the disease development. [ABSTRACT FROM AUTHOR]

Published

2018

6. High throughput profiling of whole plasma N-glycans in type II diabetes mellitus patients and healthy individuals: A perspective from a Ghanaian population.

Author

Adua, Eric, Memarian, Elham, Russell, Alyce, Trbojević-Akmačić, Irena, Gudelj, Ivan, Jurić, Julija, Roberts, Peter, Lauc, Gordan, and Wang, Wei

Subjects

*TYPE 2 diabetes, *GHANAIANS, *CELL metabolism, *BIOLOGICAL tags, *CROSS-sectional method

Abstract

Abstract Aberrant protein glycosylation may reflect changes in cell metabolism of type II diabetes mellitus (T2DM) and offers fresh vistas for discovering potential biomarkers. However, the functional significance of T2DM N-glycan alterations is underexplored, since to date, N-glycan profiling studies have been performed in selected populations. Geographically and genetically isolated populations are needed for validation of specific biomarkers. This age-sex matched cross sectional study comprising 232 T2DM patients and 219 controls was conducted in Ghana, Western Africa. Blood plasma samples were collected for clinical assessment after which plasma N-glycans were freed and analysed by ultra-performance liquid chromatography (UPLC). High branching (HB) [W = 46328; q = 0.00072], tri-galactosylated (G3) [W = 44076; q = 0.00096], antennary fucosylated (FUC_A) [W = 43055; q = 0.0000763], and triantennary (TRIA) [W = 44624; q = 0.0025], N-glycan structures were increased in T2DM whereas low branching (LB) [W = 46328; q = 0.00072], non-sialylated (S0) [W = 46929; q = 0.00292], monogalactosylation (G1) [W = 44091; q = 0.0000763], core fucosylation (FUC_C), [W = 46497; q = 0.00096], biantennary galactosylation (A2G) [W = 45663; q = 0.000763], and biantennary (BA) [W = 46376; q = 0.00072], structures were decreased compared to controls. Nine N-glycan peaks (GPs (GP1, GP4, GP7, GP11, GP17, GP19, GP22, GP26, GP29)) were found to predict case status based on Akaike's information criterion (AIC) and Bayesian information criterion (BIC) model selection. Adjusting for age, sex and other co-variates in this model yielded an area under the curve (AUC) of 80.5% with sensitivity of 79% and specificity of 73%, indicating the predicting power of N-glycans as robust biomarkers. Our results show that hyperglycemia influences N-glycan complexities among Ghanaians. N-glycan profiling in distinct populations has affirmed the potentiality of N-glycan profiles as generic biomarkers which may facilitate better prognosis for T2DM. Highlights • T2DM was associated with a decreased core fucosylated plasma N-glycans. • T2DM was associated with decreased low-branching plasma N-glycans. • T2DM was associated with increased high branching plasma N-glycans. • T2DM was associated with increased disialylated and trisialylated plasma N-glycans. • The area under the curve was 80.5% indicating the good predicting power of N-glycans. [ABSTRACT FROM AUTHOR]

Published

2019