Your search keyword '"Rasic, Milica"' showing total 8 results

1. Genetic polymorphisms and Methotrexate response in patients with rheumatoid arthritis.

Author

GRK, Milka, JEKIC, Biljana, DOLZAN, Vita, MAKSIMOVIC, Nela, DAMNJANOVIC, Tatjana, RASIC, Milica, NOVAKOVIC, Ivana, PEROVIC, Dijana, CARKIC, Jelena, and DUSANOVIC PJEVIC, Marija

Subjects

MATRIX metalloproteinases, GENETIC variation, GENETIC polymorphisms, RHEUMATOID arthritis, EXTRACELLULAR enzymes

Abstract

In the context of rheumatoid arthritis (RA) treatment, Methotrexate (MTX) plays a crucial role in preventing joint damage and bone erosion (BE). RA is characterized by elevated levels of matrix metalloproteinase 2 (MMP2), an enzyme responsible for extracellular matrix degradation, which contributes to joint damage and inflammation. Tissue inhibitor of metalloproteinase 2 (TIMP2) counteracts MMP2, and an imbalance between the two can exacerbate BE. Inosine triphosphatase (ITPA) is an enzyme involved in regulating inosine triphosphate levels, potentially linked to RA susceptibility. Genetic variations in ITPA, MMP2, and TIMP2 genes can influence MTX's efficacy. A study of 122 RA patients on MTX monotherapy assessed its effectiveness using Disease Activity Score (DAS28) changes over 6 months following EULAR response criteria. Genotyping, including MMP2 (rs243866, rs2285053), TIMP2 (rs2277698), and ITPA (rs1127354) polymorphisms, was performed. Among the patients, 87.7% were responders, 63.9% experienced BE, and 24.6% encountered adverse events. Notably, patients with the MMP2 (rs243866) GG genotype were the only ones reporting nausea (p=0.025). Patients with both the MMP2 (rs2285053) CC and TIMP2 (rs2277698) CT genotypes had a lower incidence of BE compared to those lacking this combination (p=0.048). The TIMP2 (rs2277698) CC genotype was associated with a higher baseline DAS28 score (p=0.035). In summary, this study suggests that specific MMP2/TIMP2 genotype combinations may serve as predictors for BE development in RA patients undergoing MTX monotherapy. [ABSTRACT FROM AUTHOR]

Published

2024

2. Association of IL-6 rs1800795, but not TNF-α rs1800629, and IL-1β rs16944 polymorphisms' genotypes with recovery of ischemic stroke patients following thrombolysis.

Author

Dusanovic Pjevic, Marija, Vojvodic, Ljubica, Grk, Milka, Todorovic, Jovana, Maksimovic, Nela, Rasic, Milica, Perovic, Dijana, Damnjanovic, Tatjana, Trickovic, Jelena, Kacar, Katarina, and Jekic, Biljana

Subjects

ISCHEMIC stroke, STROKE patients, TISSUE plasminogen activator, GENOTYPES, INTERLEUKIN-6, STROKE

Abstract

Inflammatory cytokines like tumor necrosis factor-α (TNF-α), interleukin (IL)-1β, and IL-6 can cause brain injury, slow recovery, and adverse effects (ADEs) in ischemic stroke (IS) patients treated with recombinant tissue plasminogen activator (rtPA). We explored the relationship between selected polymorphisms within TNF-α, IL-1β and IL-6 genes, and post-IS outcome and ADEs in patients treated with rtPA. One hundred and sixty-six patients with IS treated with rtPA were included in this study. The modified Rankin Scale (mRS) was used to assess functional recovery 3 months after IS likewise thrombolytic therapy efficacy. Patients were classified into groups with favorable (0–1) or poor recovery based on their mRS score at the ninetieth day post-IS. During hospitalization, ADEs following rtPA were monitored. TNF-α-308 G/A (rs1800629), IL-1β-511 G/A (rs16944), and IL-6-174 G/C (rs1800795) polymorphisms were genotyped using Real-Time PCR. SPSS software version 22.0 was used for statistical analyses. Patients with the TNF-α-308 G/A GG genotype had a higher mean NIHSS value at admission (12.75 ± 5.176) than those carrying A-allele (10.56 ± 3.979;p = 0.016). Individuals with the CC genotype of the IL-6-174 G/C polymorphism had significantly lower NIHSS scores (8.79 ± 5.053) than those with G-allele (12.06 ± 6.562) 24 hours after rtPA (p = 0.050). Patients with the GG genotype of the IL-6-174 G/C polymorphism had a significantly poorer outcome (p = 0.024; OR = 2.339; 95%CI 1.121–4.880), while patients who were G-allele carriers of the Il-6–174 G/C polymorphism and had the AA genotype of the IL-1β-511 G/A polymorphism were statistically significantly more likely to experience hemorrhagic transformation (p = 0.046; OR = 2.7273; 95%CI 1.0414–7.1426). GG genotype of the IL-6-174 G/C polymorphism is associated with poor recovery after IS treated with rtPA therapy. [ABSTRACT FROM AUTHOR]

Published

2024

3. Targeting B7-H3—A Novel Strategy for the Design of Anticancer Agents for Extracranial Pediatric Solid Tumors Treatment

Author

Rasic, Petar, primary, Jeremic, Marija, additional, Jeremic, Rada, additional, Dusanovic Pjevic, Marija, additional, Rasic, Milica, additional, Djuricic, Slavisa M., additional, Milickovic, Maja, additional, Vukadin, Miroslav, additional, Mijovic, Tanja, additional, and Savic, Djordje, additional

Published

2023

4. Chromosomal microarray in postnatal diagnosis of congenital anomalies and neurodevelopmental disorders in Serbian patients

Author

Perovic, Dijana, primary, Damnjanovic, Tatjana, additional, Jekic, Biljana, additional, Dusanovic‐Pjevic, Marija, additional, Grk, Milka, additional, Djuranovic, Ana, additional, Rasic, Milica, additional, Novakovic, Ivana, additional, and Maksimovic, Nela, additional

Published

2022

5. Organic thiocyanates - glucosinolate enzymatic degradation products or artefacts of the isolation procedure?

Author

Todorovska-Rasic, Milica, primary and Radulovic, Niko, additional

Published

2020

6. Origin as a grimase: Nietzsche's view of genealogy

Author

Rasic, Milica, primary

Published

2015

7. Load modelling at low voltage using continuous measurements

Author

Korunovic, Lidija, primary, Rasic, Milica, additional, Floranovic, Nenad, additional, and Aleksic, Vladica, additional

Published

2014

8. B7 homolog 3 in pancreatic cancer.

Author

Perovic D, Dusanovic Pjevic M, Perovic V, Grk M, Rasic M, Milickovic M, Mijovic T, and Rasic P

Subjects

Humans, Animals, Drug Resistance, Neoplasm immunology, Immune Checkpoint Inhibitors therapeutic use, Immune Checkpoint Inhibitors pharmacology, Immunotherapy methods, Antineoplastic Agents, Immunological therapeutic use, Antibodies, Monoclonal therapeutic use, Pancreatic Neoplasms immunology, Pancreatic Neoplasms pathology, Pancreatic Neoplasms therapy, Pancreatic Neoplasms drug therapy, Pancreatic Neoplasms metabolism, Pancreatic Neoplasms mortality, B7 Antigens metabolism, B7 Antigens antagonists & inhibitors, B7 Antigens immunology

Abstract

Despite advances in cancer treatment, pancreatic cancer (PC) remains a disease with high mortality rates and poor survival outcomes. The B7 homolog 3 (B7-H3) checkpoint molecule is overexpressed among many malignant tumors, including PC, with low or absent expression in healthy tissues. By modulating various immunological and nonimmunological molecular mechanisms, B7-H3 may influence the progression of PC. However, the impact of B7-H3 on the survival of patients with PC remains a subject of debate. Still, most available scientific data recognize this molecule as a suppressive factor to antitumor immunity in PC. Furthermore, it has been demonstrated that B7-H3 stimulates the migration, invasion, and metastasis of PC cells, and enhances resistance to chemotherapy. In preclinical models of PC, B7-H3-targeting monoclonal antibodies have exerted profound antitumor effects by increasing natural killer cell-mediated antibody-dependent cellular cytotoxicity and delivering radioisotopes and cytotoxic drugs to the tumor site. Finally, PC treatment with B7-H3-targeting antibody-drug conjugates and chimeric antigen receptor T cells is being tested in clinical studies. This review provides a comprehensive analysis of all PC-related studies in the context of B7-H3 and points to deficiencies in the current data that should be overcome by future research., Competing Interests: Conflict-of-interest statement: All the authors report no relevant conflicts of interest for this article., (©The Author(s) 2024. Published by Baishideng Publishing Group Inc. All rights reserved.)

Published

2024