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Authors = Gytis Svirskis

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19 pages, 3824 KiB  
Article
Comparison of Microglial Morphology and Function in Primary Cerebellar Cell Cultures on Collagen and Collagen-Mimetic Hydrogels
by Zbigniev Balion, Nataša Svirskienė, Gytis Svirskis, Hermanas Inokaitis, Vytautas Cėpla, Artūras Ulčinas, Tadas Jelinskas, Romuald Eimont, Neringa Paužienė, Ramūnas Valiokas and Aistė Jekabsone
Biomedicines 2022, 10(5), 1023; https://doi.org/10.3390/biomedicines10051023 - 29 Apr 2022
Cited by 6 | Viewed by 3673
Abstract
Neuronal-glial cell cultures are usually grown attached to or encapsulated in an adhesive environment as evenly distributed networks lacking tissue-like cell density, organization and morphology. In such cultures, microglia have activated amoeboid morphology and do not display extended and intensively branched processes characteristic [...] Read more.
Neuronal-glial cell cultures are usually grown attached to or encapsulated in an adhesive environment as evenly distributed networks lacking tissue-like cell density, organization and morphology. In such cultures, microglia have activated amoeboid morphology and do not display extended and intensively branched processes characteristic of the ramified tissue microglia. We have recently described self-assembling functional cerebellar organoids promoted by hydrogels containing collagen-like peptides (CLPs) conjugated to a polyethylene glycol (PEG) core. Spontaneous neuronal activity was accompanied by changes in the microglial morphology and behavior, suggesting the cells might play an essential role in forming the functional neuronal networks in response to the peptide signalling. The present study examines microglial cell morphology and function in cerebellar cell organoid cultures on CLP-PEG hydrogels and compares them to the cultures on crosslinked collagen hydrogels of similar elastomechanical properties. Material characterization suggested more expressed fibril orientation and denser packaging in crosslinked collagen than CLP-PEG. However, CLP-PEG promoted a significantly higher microglial motility (determined by time-lapse imaging) accompanied by highly diverse morphology including the ramified (brightfield and confocal microscopy), more active Ca2+ signalling (intracellular Ca2+ fluorescence recordings), and moderate inflammatory cytokine level (ELISA). On the contrary, on the collagen hydrogels, microglial cells were significantly less active and mostly round-shaped. In addition, the latter hydrogels did not support the neuron synaptic activity. Our findings indicate that the synthetic CLP-PEG hydrogels ensure more tissue-like microglial morphology, motility, and function than the crosslinked collagen substrates. Full article
(This article belongs to the Special Issue Biomedical Properties of Hydrogels)
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19 pages, 2541 KiB  
Article
Effects of Metformin on Spontaneous Ca2+ Signals in Cultured Microglia Cells under Normoxic and Hypoxic Conditions
by Silvija Jankeviciute, Natasa Svirskiene, Gytis Svirskis and Vilmante Borutaite
Int. J. Mol. Sci. 2021, 22(17), 9493; https://doi.org/10.3390/ijms22179493 - 31 Aug 2021
Cited by 4 | Viewed by 2873
Abstract
Microglial functioning depends on Ca2+ signaling. By using Ca2+ sensitive fluorescence dye, we studied how inhibition of mitochondrial respiration changed spontaneous Ca2+ signals in soma of microglial cells from 5–7-day-old rats grown under normoxic and mild-hypoxic conditions. In microglia under [...] Read more.
Microglial functioning depends on Ca2+ signaling. By using Ca2+ sensitive fluorescence dye, we studied how inhibition of mitochondrial respiration changed spontaneous Ca2+ signals in soma of microglial cells from 5–7-day-old rats grown under normoxic and mild-hypoxic conditions. In microglia under normoxic conditions, metformin or rotenone elevated the rate and the amplitude of Ca2+ signals 10–15 min after drug application. Addition of cyclosporin A, a blocker of mitochondrial permeability transition pore (mPTP), antioxidant trolox, or inositol 1,4,5-trisphosphate receptor (IP3R) blocker caffeine in the presence of rotenone reduced the elevated rate and the amplitude of the signals implying sensitivity to reactive oxygen species (ROS), and involvement of mitochondrial mPTP together with IP3R. Microglial cells exposed to mild hypoxic conditions for 24 h showed elevated rate and increased amplitude of Ca2+ signals. Application of metformin or rotenone but not phenformin before mild hypoxia reduced this elevated rate. Thus, metformin and rotenone had the opposing fast action in normoxia after 10–15 min and the slow action during 24 h mild-hypoxia implying activation of different signaling pathways. The slow action of metformin through inhibition of complex I could stabilize Ca2+ homeostasis after mild hypoxia and could be important for reduction of ischemia-induced microglial activation. Full article
(This article belongs to the Special Issue Metformin: The Scope for New Applications)
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24 pages, 6528 KiB  
Article
Cerebellar Cells Self-Assemble into Functional Organoids on Synthetic, Chemically Crosslinked ECM-Mimicking Peptide Hydrogels
by Zbigniev Balion, Vytautas Cėpla, Nataša Svirskiene, Gytis Svirskis, Kristina Druceikaitė, Hermanas Inokaitis, Justina Rusteikaitė, Ignas Masilionis, Gintarė Stankevičienė, Tadas Jelinskas, Artūras Ulčinas, Ayan Samanta, Ramūnas Valiokas and Aistė Jekabsone
Biomolecules 2020, 10(5), 754; https://doi.org/10.3390/biom10050754 - 12 May 2020
Cited by 32 | Viewed by 7091
Abstract
Hydrogel-supported neural cell cultures are more in vivo-relevant compared to monolayers formed on glass or plastic substrates. However, there is a lack of synthetic microenvironment available for obtaining standardized and easily reproducible cultures characterized by tissue-mimicking cell composition, cell–cell interactions, and functional networks. [...] Read more.
Hydrogel-supported neural cell cultures are more in vivo-relevant compared to monolayers formed on glass or plastic substrates. However, there is a lack of synthetic microenvironment available for obtaining standardized and easily reproducible cultures characterized by tissue-mimicking cell composition, cell–cell interactions, and functional networks. Synthetic peptides representing the biological properties of the extracellular matrix (ECM) proteins have been reported to promote the adhesion-driven differentiation and functional maturation of neural cells. Thus, such peptides can serve as building blocks for engineering a standardized, all-synthetic environment. In this study, we have compared the effect of two chemically crosslinked hydrogel compositions on primary cerebellar cells: collagen-like peptide (CLP), and CLP with an integrin-binding motif arginine-glycine-aspartate (CLP-RGD), both conjugated to polyethylene glycol molecular templates (PEG-CLP and PEG-CLP-RGD, respectively) and fabricated as self-supporting membranes. Both compositions promoted a spontaneous organization of primary cerebellar cells into tissue-like clusters with fast-rising Ca2+ signals in soma, reflecting action potential generation. Notably, neurons on PEG-CLP-RGD had more neurites and better synaptic efficiency compared to PEG-CLP. For comparison, poly-L-lysine-coated glass and plastic surfaces did not induce formation of such spontaneously active networks. Additionally, contrary to the hydrogel membranes, glass substrates functionalized with PEG-CLP and PEG-CLP-RGD did not sufficiently support cell attachment and, subsequently, did not promote functional cluster formation. These results indicate that not only chemical composition but also the hydrogel structure and viscoelasticity are essential for bioactive signaling. The synthetic strategy based on ECM-mimicking, multifunctional blocks in registry with chemical crosslinking for obtaining tissue-like mechanical properties is promising for the development of fast and well standardized functional in vitro neural models and new regenerative therapies. Full article
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7 pages, 269 KiB  
Article
The scientific heritage of Professor Aron Gutman (Commemorating the 10th anniversary of Aron Gutman’s death)
by Armuntas Baginskas, Gytis Svirskis and Rimvydas Miliauskas
Medicina 2009, 45(9), 732; https://doi.org/10.3390/medicina45090096 - 21 Sep 2009
Cited by 2 | Viewed by 1017
Abstract
Aron Gutman started his scientific research when he was a student of the Department of Physics and Mathematics, Vilnius University. At that time, he developed the theory of nonhomogenous vector relations between magnetic moments of electrons in an atom and applied it for [...] Read more.
Aron Gutman started his scientific research when he was a student of the Department of Physics and Mathematics, Vilnius University. At that time, he developed the theory of nonhomogenous vector relations between magnetic moments of electrons in an atom and applied it for explanation of energy spectrum of real atoms. Since 1960, he worked in Kaunas Medical Institute, and his main field of scientific interests was theoretical biophysics and electrophysiology of living tissues and cells. The earlier biophysical works of A. Gutman dealt with problems of the bioelectrical fields that underlie electroencephalogram, electrocorticogram, and electrocardiogram. The most important achievement was a theory of individual potential or postsynaptic field potential of synapses from individual axon (EEG quantum) and its role in shaping of electroencephalogram. In the later works (from 1971), he looked into properties and function of the individual nerve cells. He had created and developed the theory of nonlinear (bistable) dendrites and analyzed functional implications of such dendrites. In the last works, A. Gutman tried to relate the functioning of the nervous system at the cellular and system levels. He made efforts to find connection between the properties of individual neurones and principles (laws) of functioning of the nervous system. He had managed to relate dendritic bistability of neurones and Gelfand-Tsetlin principle of the functioning of the central nervous system (also known as the principle of minimal afferentiation). He explained some regularities in motor control by the dendritic bistability of motoneurones. Full article
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