Your search keyword '"Iwona Pelikant‐Małecka"' showing total 9 results

1. Mesenchymal stem cells transfer mitochondria to allogeneic Tregs in an HLA-dependent manner improving their immunosuppressive activity

Author

Karolina Piekarska, Zuzanna Urban-Wójciuk, Małgorzta Kurkowiak, Iwona Pelikant-Małecka, Adriana Schumacher, Justyna Sakowska, Jan Henryk Spodnik, Łukasz Arcimowicz, Hanna Zielińska, Bogusław Tymoniuk, Alicja Renkielska, Janusz Siebert, Ewa Słomińska, Piotr Trzonkowski, Ted Hupp, and Natalia Maria Marek-Trzonkowska

Subjects

Science

Abstract

Regulatory T (Treg) cells and mesenchymal stem cells (MSCs) are both cell populations capable of immune tolerance induction. Here the authors show that the transfer of mitochondria from mesenchymal stem cells to allogeneic Treg cells in an HLA-dependent manner results in enhanced immunosuppressive functions of Treg cells.

Published

2022

2. DNA methylation profile in patients with indolent systemic mastocytosis

Author

Aleksandra Górska, Ewa Jabłońska, Edyta Reszka, Marek Niedoszytko, Magdalena Lange, Marta Gruchała‐Niedoszytko, Justyna Jarczak, Dominik Strapagiel, Magdalena Górska‐Ponikowska, Paulina Bastian, Iwona Pelikant‐Małecka, Leszek Kalinowski, and Bogusław Nedoszytko

Subjects

DNA methylation, epigenetics, KIT mutation, mastocytosis, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract Background Mastocytosis is a clinically heterogeneous, usually acquired disease of the mast cells with a survival time that depends on the onset of the disease and ranges from skin‐limited to systemic disease, including indolent and more aggressive variants. The crucial element in pathogenesis is the presence of oncogenic KIT somatic mutation D816V. Further epigenetic alterations are responsible for regulating the expression of genes. It is essential to identify indicators of disease progression, and the specific clinical picture to establish an appropriate therapeutic strategy. Objective The aim of this study was to analyze the relation of mastocytosis symptoms and epigenetic changes, and to identify epigenetic predictors of the disease. Methods Global DNA methylation profile analysis was performed in peripheral blood collected from 73 patients with indolent systemic mastocytosis (ISM) and 43 healthy adult volunteers. Levels of 5‐methylcytosine (5‐mC) and 5‐hydroxymethylcytosine (5‐hmC) were determined using an ELISA‐based method, while the methylation of the Alu and LINE‐1 repeats were assayed with the quantitative methylation‐specific PCR technique. A questionnaire interview was conducted among the study participants to collect data on possible epigenetic modifiers. Additionally, the methylation profile was compared between three human mast cell lines: ROSA KIT D816V, ROSA KIT WT, and HMC‐1.1 KIT V560G, in order to assess the association between KIT mutations and methylation profile. Results A significantly lower level of DNA hydroxymethylation (5‐hmC) in the blood was found in patients with ISM as compared to the controls (0.022% vs. 0.042%, p = 0.0001). Differences in the markers of global DNA methylation (5‐mC, Alu, LINE‐1) were not statistically significant, although they did indicate generally higher DNA methylation in patients with mastocytosis. The 5‐hmC level was significantly associated with allergy (p = 0.011) in patients with ISM, showing a higher level of 5‐hmC in patients with allergy as compared to patients without allergy. The in vitro study revealed significant differences between the studied cell lines at the level of 5‐mC, Alu, and LINE‐1. Conclusions This study confirms that epigenetic changes are involved in mastocytosis, and suggests that allergy may be an important epigenetic modifier of the disease. A possible association between KIT mutations and methylation status observed in human mast cell lines requires further investigation in human studies. Clinical Implications Epigenetic alterations are involved in mastocytosis pathology. The possible role of allergy as an important epigenetic modifier suggests the more impaired function of mast cells in ISM patients without allergy. Capsule summary Decreased DNA demethylation in the blood DNA of patients with ISM confirms that epigenetic alterations are involved in mastocytosis pathology. We observed a possible role of allergy as an important epigenetic modifier. There is a possible association between KIT mutations and the methylation status observed in human mast cell lines.

Published

2021

3. Proteomic and Metabolomic Changes in Psoriasis Preclinical and Clinical Aspects

Author

Adrianna Radulska, Iwona Pelikant-Małecka, Kamila Jendernalik, Iwona T. Dobrucki, and Leszek Kalinowski

Subjects

Inorganic Chemistry, Organic Chemistry, General Medicine, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Catalysis, Computer Science Applications

Abstract

Skin diseases such as psoriasis (Ps) and psoriatic arthritis (PsA) are immune-mediated inflammatory diseases. Overlap of autoinflammatory and autoimmune conditions hinders diagnoses and identifying personalized patient treatments due to different psoriasis subtypes and the lack of verified biomarkers. Recently, proteomics and metabolomics have been intensively investigated in a broad range of skin diseases with the main purpose of identifying proteins and small molecules involved in the pathogenesis and development of the disease. This review discusses proteomics and metabolomics strategies and their utility in research and clinical practice in psoriasis and psoriasis arthritis. We summarize the studies, from in vivo models conducted on animals through academic research to clinical trials, and highlight their contribution to the discovery of biomarkers and targets for biological drugs.

Published

2023

4. Simultaneous activation of mGlu

Author

Paulina, Cieślik, Helena, Domin, Agnieszka, Chocyk, Piotr, Gruca, Ewa, Litwa, Agata, Płoska, Adrianna, Radulska, Iwona, Pelikant-Małecka, Piotr, Brański, Leszek, Kalinowski, and Joanna M, Wierońska

Subjects

Male, Sulfonamides, Receptor, Muscarinic M5, Dose-Response Relationship, Drug, Pyridines, Receptor, Muscarinic M1, Receptors, Metabotropic Glutamate, Rats, Mice, Animals, Cognitive Dysfunction, Dizocilpine Maleate, Rats, Wistar, Excitatory Amino Acid Antagonists

Abstract

The activity of an allosteric agonist of muscarinic M

Published

2019

5. Simultaneous activation of muscarinic and GABA

Author

Paulina, Cieślik, Monika, Woźniak, Krzysztof, Tokarski, Magdalena, Kusek, Andrzej, Pilc, Agata, Płoska, Adrianna, Radulska, Iwona, Pelikant-Małecka, Beata, Żołnowska, Jarosław, Sławiński, Leszek, Kalinowski, and Joanna M, Wierońska

Subjects

Male, Neurotransmitter Agents, Indoles, Pyridines, Brain, Excitatory Postsynaptic Potentials, Cyclopentanes, Thiophenes, Receptors, Muscarinic, Disease Models, Animal, Mice, Pyrimidines, Allosteric Regulation, Receptors, GABA-B, Benzamides, Schizophrenia, Animals, Drug Therapy, Combination, Antipsychotic Agents

Abstract

Recent preclinical studies point to muscarinic and GABA

Published

2018

6. Abstracts from Purines 2014, an International Conference on Nucleotides, Nucleosides and Nucleobases, held in Bonn, Germany, from July 23–27, 2014

Author

Henrique Silva, Gary Housley, Mireia Medrano, Feranando Cagide, Alexandra Gaspar, Iwona Pelikant-Małecka, ROCCHINA LUCIA COLUCCI, Maria Adelina Coelho Costa, Margarida Duarte Cerqueira Martins de Araújo, Isabel Calejo, José Bernardo Noronha-Matos, Rafael Ferreira Soares, João Lopes, Gennady Yegutkin, Manuel Izquierdo, Nélio Da Mota Gonçalves, and Maija Hollmén

Subjects

Agonist, 0303 health sciences, Chemistry, medicine.drug_class, Adenosine A2A receptor, Inflammation, Cell Biology, Pharmacology, Fibroblast growth factor, 01 natural sciences, Article, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, 03 medical and health sciences, Cellular and Molecular Neuroscience, Tissue expression, Edema, medicine, medicine.symptom, Molecular Biology, 030304 developmental biology

Published

2014

7. Hidden Pool of Cardiac Adenine Nucleotides That Controls Adenosine Production

Author

Magdalena A. Zabielska-Kaczorowska, Alicja Braczko, Iwona Pelikant-Malecka, Ewa M. Slominska, and Ryszard T. Smolenski

Subjects

adenosine, rat heart, ischemia, contractility, ATP, nucleotide catabolites, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Myocardial ischemic adenosine production decreases in subsequent events that may blunt its protective functions. To test the relation between total or mitochondrial cardiac adenine nucleotide pool (TAN) on the energy status with adenosine production, Langendorff perfused rat hearts were subjected to three protocols: 1 min ischemia at 40 min, 10 min ischemia at 50 min, and 1 min ischemia at 85 min in Group I; additional infusion of adenosine (30 µM) for 15 min after 10 min ischemia in Group I-Ado, and 1 min ischemia at 40 and 85 min in the controls (Group No I). A 31P NMR and an HPLC were used for the analysis of nucleotide and catabolite concentrations in the heart and coronary effluent. Cardiac adenosine production in Group I measured after 1 min ischemia at 85 min decreased to less than 15% of that at 40 min in Group I, accompanied by a decrease in cardiac ATP and TAN to 65% of the initial results. Adenosine production at 85 min was restored to 45% of that at 40 min in Group I-Ado, accompanied by a rebound of ATP and TAN by 10% vs. Group I. Mitochondrial TAN and free AMP concentrations paralleled that of total cardiac TAN. Changes in energy equilibrium or mitochondrial function were minor. This study highlights that only a fraction of the cardiac adenine nucleotide pool is available for adenosine production, but further studies are necessary to clarify its nature.

Published

2023

8. Chloroacridine derivatives as potential anticancer agents which may act as tricarboxylic acid cycle enzyme inhibitors

Author

Miroslawa Cichorek, Anna Ronowska, Krystyna Dzierzbicka, Monika Gensicka-Kowalewska, Milena Deptula, and Iwona Pelikant-Malecka

Subjects

Chloroacridine, Amelanotic melanoma, Melanotic melanoma, Apoptosis, Tricarboxylic acid cycle enzymes, Cell death, Therapeutics. Pharmacology, RM1-950

Abstract

Purpose: This paper concerns the cytotoxicity of 9-chloro-1-nitroacridine (1a) and 9-chloro-4-methyl-1-nitroacridine (1b) against two biologically different melanoma forms: melanotic and amelanotic. Melanomas are tumors characterized by high heterogeneity and poor susceptibility to chemotherapies. Among new analogs synthesized by us, compound 1b exhibited the highest anticancer potency. Because of that, in this study, we analyzed the mechanism of action for 1a and its 4-methylated derivative, 1b, against a pair of biological melanoma forms, with regard to proliferation, cell death mechanism and energetic state. Methods: Cytotoxicity was evaluated by XTT assay. Cell death was estimated by plasma membrane structure changes (phosphatidylserine externalization), caspase activation, and ROS presence. The energetic state of cells was estimated based on NAD and ATP levels, and the activity of tricarboxylic acid cycle enzymes (pyruvate dehydrogenase complex, aconitase, isocitrate dehydrogenase). Results: The chloroacridines affect biological forms of melanoma in different ways. Amelanotic (Ab) melanoma (with inhibited melanogenesis and higher malignancy) was particularly sensitive to the action of the chloroacridines. The Ab melanoma cells died through apoptosis and through death without caspase activation. Diminished activity of TAC enzymes was noticed among Ab melanoma cells together with ATP/NAD depletion, especially in the case of 1b. Conclusion: Our data show that the biological forms of the tumors responded to 1a and its 4-methylated analog in different ways. 1a and 1b could be inducers of regulated melanoma cell death, especially the amelanotic form. Although the mechanism of the cell death is not fully understood, 1b may act by interfering with the TAC enzymes and blocking specific pathways leading to tumor growth. This could encourage further investigation of its anticancer activity, especially against the amelanotic form of melanoma.

Published

2020

9. Gender-Related Differences in Trimethylamine and Oxidative Blood Biomarkers in Cardiovascular Disease Patients

Author

Laura Bordoni, Donatella Fedeli, Marco Piangerelli, Iwona Pelikant-Malecka, Adrianna Radulska, Joanna J. Samulak, Angelika K. Sawicka, Lukasz Lewicki, Leszek Kalinowski, Robert A. Olek, and Rosita Gabbianelli

Subjects

gender, membrane erythrocyte, hydroperoxides, biomarker, DPPP, DPH, Biology (General), QH301-705.5

Abstract

Gender differences in the burden of cardiovascular disease (CVD) have been observed worldwide. In this study, plasmatic levels of trimethylamine (TMA) and blood oxidative biomarkers have been evaluated in 358 men (89 controls and 269 CVD patients) and 189 women (64 control and 125 CVD patients). The fluorescence technique was applied to determine erythrocyte membrane fluidity using 1,6-diphenyl-1,3,5-hexatriene (DPH) and Laurdan, while lipid hydroperoxides were assessed by diphenyl−1-pyrenylphosphine (DPPP). Results show that levels of plasmatic TMA were higher in healthy men with respect to healthy women (p = 0.0001). Significantly lower TMA was observed in male CVD patients (0.609 ± 0.104 μM) compared to healthy male controls (0.680 ± 0.118 μM) (p < 0.001), while higher levels of TMA were measured in female CVD patients (0.595 ± 0.115 μM) with respect to female controls (0.529 ± 0.073 μM) (p < 0.001). DPPP was significantly higher in healthy control men than in women (p < 0.001). Male CVD patients displayed a lower value of DPPP (2777 ± 1924) compared to healthy controls (5528 ± 2222) (p < 0.001), while no significant changes were measured in females with or without CVD (p > 0.05). Membrane fluidity was significantly higher (p < 0.001) in the hydrophobic bilayer only in control male subjects. In conclusion, gender differences were observed in blood oxidative biomarkers, and DPPP value might be suggested as a biomarker predictive of CVD only in men.

Published

2020