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Browsing by Author "Robajac, Dragana (36651587600)"

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    Albumin at the intersection between antioxidant and pro-oxidant in patients on peritoneal dialysis
    (2022)
    Baralić, Marko (56258718700)
    ;
    Spasojević, Ivan (58188331900)
    ;
    Miljuš, Goran (36651540800)
    ;
    Šunderić, Miloš (55581497300)
    ;
    Robajac, Dragana (36651587600)
    ;
    Dobrijević, Zorana (55508308800)
    ;
    Gligorijević, Nikola (56088660000)
    ;
    Nedić, Olgica (7003642048)
    ;
    Penezić, Ana (57218439363)
    Albumin (HSA) is a multifunctional protein and due to its free Cys34 thiol group, represents a main source of free thiols in the circulation. This property of HSA, combined with its ability to sequester redox active Cu(II) ions, makes HSA a dominant circulatory antioxidant. End stage kidney disease (ESRD) is a condition accompanied by elevated oxidative stress. The aim of the present study was to examine changes in the antioxidative capacity of HSA and Cu(II) binding affinity in patients on peritoneal dialysis (PD), and relate it to the Cys34 thiol group content and other structural changes of this molecule. HSA molecules are modified in ESRD patients subjected to PD, having significantly lower thiol group and bound Cu(II) content, reduced antioxidant capacity, an increased content of advanced glycation end-products and altered conformation. Also, Cu(II) binding capacity of HSA in these patients is impaired, since a significant portion of the high-affinity metal-binding site is unable to interact with Cu(II). Taking into account that the concentration of Cu(II) in the circulation of ESRD patients is much higher than in healthy persons and that Cu(II) binding capacity of HSA in these patients is significantly impaired, HSA may be considered as a novel circulatory pro-oxidant, thus exacerbating oxidative stress. © 2022 Elsevier Inc.
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    Albumin at the intersection between antioxidant and pro-oxidant in patients on peritoneal dialysis
    (2022)
    Baralić, Marko (56258718700)
    ;
    Spasojević, Ivan (58188331900)
    ;
    Miljuš, Goran (36651540800)
    ;
    Šunderić, Miloš (55581497300)
    ;
    Robajac, Dragana (36651587600)
    ;
    Dobrijević, Zorana (55508308800)
    ;
    Gligorijević, Nikola (56088660000)
    ;
    Nedić, Olgica (7003642048)
    ;
    Penezić, Ana (57218439363)
    Albumin (HSA) is a multifunctional protein and due to its free Cys34 thiol group, represents a main source of free thiols in the circulation. This property of HSA, combined with its ability to sequester redox active Cu(II) ions, makes HSA a dominant circulatory antioxidant. End stage kidney disease (ESRD) is a condition accompanied by elevated oxidative stress. The aim of the present study was to examine changes in the antioxidative capacity of HSA and Cu(II) binding affinity in patients on peritoneal dialysis (PD), and relate it to the Cys34 thiol group content and other structural changes of this molecule. HSA molecules are modified in ESRD patients subjected to PD, having significantly lower thiol group and bound Cu(II) content, reduced antioxidant capacity, an increased content of advanced glycation end-products and altered conformation. Also, Cu(II) binding capacity of HSA in these patients is impaired, since a significant portion of the high-affinity metal-binding site is unable to interact with Cu(II). Taking into account that the concentration of Cu(II) in the circulation of ESRD patients is much higher than in healthy persons and that Cu(II) binding capacity of HSA in these patients is significantly impaired, HSA may be considered as a novel circulatory pro-oxidant, thus exacerbating oxidative stress. © 2022 Elsevier Inc.
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    Biochemical Markers in the Prediction of Pregnancy Outcome in Gestational Diabetes Mellitus
    (2024)
    Mandić-Marković, Vesna (23991079100)
    ;
    Dobrijević, Zorana (55508308800)
    ;
    Robajac, Dragana (36651587600)
    ;
    Miljuš, Goran (36651540800)
    ;
    Šunderić, Miloš (55581497300)
    ;
    Penezić, Ana (57218439363)
    ;
    Nedić, Olgica (7003642048)
    ;
    Ardalić, Danijela (6506626952)
    ;
    Miković, Željko (7801694296)
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    Radojičić, Ognjen (57223969149)
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    Mandić, Milica (58117641400)
    ;
    Mitrović, Jelena (58117140500)
    Background and Objectives: Gestational diabetes mellitus (GDM) may impact both maternal and fetal/neonatal health. The identification of prognostic indicators for GDM may improve risk assessment and selection of patient for intensive monitoring. The aim of this study was to find potential predictors of adverse pregnancy outcome in GDM and normoglycemic patients by comparing the levels of different biochemical parameters and the values of blood cell count (BCC) between GDM and normoglycemic patients and between patients with adverse and good outcome. Materials and Methods: Prospective clinical study included 49 patients with GDM (study group) and 44 healthy pregnant women (control group) who underwent oral glucose tolerance test (OGTT) at gestational age of 24–28 weeks. At the time of OGTT peripheral blood was taken for the determination of glucose levels, insulin, glycated hemoglobin, lipid status, homeostatic model assessment, BCC, iron and zinc metabolism, liver function, kidney function and inflammatory status. Each group was divided into two subgroups—normal and poor pregnancy outcome. Results: Higher RBC, hemoglobin concentration, hematocrit value, fasting glucose, uric acid and fibrinogen were found in GDM patients compared to control group. In GDM patients with poor pregnancy outcome values of fibrinogen, ALT, sedimentation rate, granulocyte and total leukocyte counts were elevated, while the serum level of zinc was significantly lower. Higher level of fibrinogen was found in normoglycemic patients with adverse pregnancy outcomes. ROC curve was constructed in order to assess fibrinogen’s biomarker potential. The established AUC value for diagnostic ROC was 0.816 (p < 0.001, 95% CI 0.691–0.941), while the AUC value for assessing fibrinogen’s potential to predict poor pregnancy outcome in GDM was 0.751 (p = 0.0096, 95% CI 0.561–0.941). Conclusions: The results of our study demonstrated that the best prognostic potential in GDM showed inflammation related parameters, identifying fibrinogen as a parameter with both diagnostic and prognostic ability. © 2024 by the authors.
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    Serum Glycome as a Diagnostic and Prognostic Factor in Gestational Diabetes Mellitus
    (2024)
    Radojičić, Ognjen (57223969149)
    ;
    Pažitná, Lucia (57216389607)
    ;
    Dobrijević, Zorana (55508308800)
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    Kundalia, Paras (58292894600)
    ;
    Kianičková, Kristina (57202129465)
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    Katrlík, Jaroslav (57193817320)
    ;
    Marković, Vesna Mandić (57218618497)
    ;
    Miković, Željko (7801694296)
    ;
    Nedić, Olgica (7003642048)
    ;
    Robajac, Dragana (36651587600)
    Abstract: Gestational diabetes mellitus (GDM) is a risk factor for both mother and fetus/neonate during and after the pregnancy. Inconsistent protocols and cumbersome screening procedures warrant the search for new and easily accessible biomarkers. We investigated a potential of serum N-glycome to differentiate between healthy pregnant women (n = 49) and women with GDM (n = 53) using a lectin-based microarray and studied the correlation between the obtained data and parameters of glucose and lipid metabolism. Four out of 15 lectins used were able to detect the differences between the control and GDM groups in fucosylation, terminal galactose/N-acetylglucosamine (Gal/GlcNAc), presence of Galα1,4Galβ1,4Glc (Gb3 antigen), and terminal α2,3-sialylation with AUC values above 60%. An increase in the Gb3 antigen and α2,3-sialylation correlated positively with GDM, whereas the amount of fucosylated glycans correlated negatively with the content of terminal Gal/GlcNAc. The content of GlcNAc oligomers correlated with the highest number of blood analytes, indices, and demographic characteristics, but failed to discriminate between the groups. The presence of terminal Gal residues correlated positively with the glucose levels and negatively with the LDL levels in the non-GDM group only. The results suggest fucosylation, terminal galactosylation, and the presence of Gb3 antigen as prediction markers of GDM. © Pleiades Publishing, Ltd. 2024.
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    Publication
    Serum Glycome as a Diagnostic and Prognostic Factor in Gestational Diabetes Mellitus
    (2024)
    Radojičić, Ognjen (57223969149)
    ;
    Pažitná, Lucia (57216389607)
    ;
    Dobrijević, Zorana (55508308800)
    ;
    Kundalia, Paras (58292894600)
    ;
    Kianičková, Kristina (57202129465)
    ;
    Katrlík, Jaroslav (57193817320)
    ;
    Marković, Vesna Mandić (57218618497)
    ;
    Miković, Željko (7801694296)
    ;
    Nedić, Olgica (7003642048)
    ;
    Robajac, Dragana (36651587600)
    Abstract: Gestational diabetes mellitus (GDM) is a risk factor for both mother and fetus/neonate during and after the pregnancy. Inconsistent protocols and cumbersome screening procedures warrant the search for new and easily accessible biomarkers. We investigated a potential of serum N-glycome to differentiate between healthy pregnant women (n = 49) and women with GDM (n = 53) using a lectin-based microarray and studied the correlation between the obtained data and parameters of glucose and lipid metabolism. Four out of 15 lectins used were able to detect the differences between the control and GDM groups in fucosylation, terminal galactose/N-acetylglucosamine (Gal/GlcNAc), presence of Galα1,4Galβ1,4Glc (Gb3 antigen), and terminal α2,3-sialylation with AUC values above 60%. An increase in the Gb3 antigen and α2,3-sialylation correlated positively with GDM, whereas the amount of fucosylated glycans correlated negatively with the content of terminal Gal/GlcNAc. The content of GlcNAc oligomers correlated with the highest number of blood analytes, indices, and demographic characteristics, but failed to discriminate between the groups. The presence of terminal Gal residues correlated positively with the glucose levels and negatively with the LDL levels in the non-GDM group only. The results suggest fucosylation, terminal galactosylation, and the presence of Gb3 antigen as prediction markers of GDM. © Pleiades Publishing, Ltd. 2024.

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