izpis_h1_title_alt

Vloga nikotinskega acetilholinskega receptorja alfa-7 pri presnovni aktivnosti izoliranih monocitov po aktivaciji z lipopolisaharidom
ID Frelih, Aljaž (Author), ID Žiberna, Lovro (Mentor) More about this mentor... This link opens in a new window, ID Kovačič, Uroš (Comentor)

.pdfPDF - Presentation file, Download (3,91 MB)
MD5: 87078F43464D5A49E2F341EDA728926D

Abstract
Monociti so ključni regulatorji vnetja in prirojene imunosti. Energijo pridobivajo preko dveh poti, glikolize in oksidativne fosforilacije. Njihova presnova je močno povezana z uravnavanjem fenotipov naslednje razvojne stopnje monocitov, makrofagov M1 in M2. Makrofagi M1 za pridobivanje energije izkoriščajo predvsem glikolizo, medtem ko se makrofagi M2 poslužujejo predvsem oksidativne fosforilacije. Aktivacija monocitov z bakterijskim lipopolisaharidom (LPS) prevesi fenotip v smer stanja M1. Z uporabo analizatorja Agilent Seahorse XFe24 smo kvantificirali stopnjo aktivnosti glikolize z merjenjem stopnje zunajcelične acidifikacije v realnem času. Ugotovili smo, da se monocitom iz periferne krvi po aktivaciji z LPS poviša stopnja zunajcelične acidifikacije, kar je skladno z rezultati drugih raziskav, ki kažejo premik presnove aktiviranih monocitov proti glikolizi. Znano je, da parasimpatična aktivacija zavira aktivacijo in sproščanje vnetnih citokinov iz makrofagov v vranici, s čimer omejuje pretiran vnetni odziv. Predpostavljamo, da acetilholin, glavni živčni prenašalec parasimpatičnega živčevja, preko α7-nikotinskih acetilholinskih receptorjev zniža glikolitično presnovno aktivnost monocitov, aktiviranih z LPS. V magistrski nalogi smo s poskusi na analizatorju Seahorse XFe24 preverili, ali inkubacija aktiviranih monocitov z neselektivnim holinergikom acetilholinom zavira njihovo glikolitično aktivnost. S specifičnimi holinergičnimi antagonisti smo ugotavljali, ali je to zaviranje povezano z učinkom acetilholina na α7 nikotinske acetilholinske receptorje. Zaradi prisotnosti nevtrofilcev v vzorcu izoliranih monocitov smo opredelili tudi njihovo presnovno aktivnost in s tem ovrednotili njihov vpliv na rezultate v našem izolatu monocitov. Naši eksperimentalni podatki kažejo, da je acetilholin šibko zaviral povečanje stopnje aktivnosti glikolize monocitov po aktivaciji z LPS. Ta učinek smo preprečili samo z α bungarotoksinom, antagonistom α7-nikotinskih acetilholinskih receptorjev, kar kaže, da acetilholin zavira presnovno aktivnost aktiviranih monocitov predvsem preko navedenih receptorjev. Statistično značilnega vpliva aktivacije z LPS na mitohondrijsko dihanje monocitov nismo zaznali. Pri poskusih na izolatu nevtrofilcev smo ugotovili, da je LPS močno povišal obseg aktivnosti tako glikolize kot tudi oksidativne fosforilacije, holinergični vpliv na te spremembe presnove pa je bil zanemarljiv.

Language:Slovenian
Keywords:α7-nikotinski acetilholinski receptor, glikoliza, glikolitično reprogramiranje, holinergična hipoteza, monocit
Work type:Master's thesis/paper
Organization:FFA - Faculty of Pharmacy
Year:2024
PID:20.500.12556/RUL-158666 This link opens in a new window
Publication date in RUL:19.06.2024
Views:55
Downloads:20
Metadata:XML RDF-CHPDL DC-XML DC-RDF
:
Copy citation
Share:Bookmark and Share

Secondary language

Language:English
Title:The role of alpha-7 nicotinic acetylcholine receptor in the metabolic activity of isolated monocytes after activation with lipopolysaccharide
Abstract:
Monocytes are key regulators of inflammation and innate immunity. They obtain energy through two pathways: glycolysis and oxidative phosphorylation. Their metabolism is closely linked to the regulation of the phenotypes of the subsequent developmental stages of monocytes, M1 and M2 macrophages. M1 macrophages primarily utilize glycolysis for energy production, while M2 macrophages primarily rely on oxidative phosphorylation. Activation of monocytes with bacterial lipopolysaccharide (LPS) shifts the phenotype towards the M1 state. Using the Agilent Seahorse XFe24 analyzer, we quantified the level of glycolytic activity by measuring the extracellular acidification rate (ECAR) in real-time. We found that peripheral blood monocytes exhibit an increased ECAR after LPS activation, which is consistent with the results of other studies showing a metabolic shift in activated monocytes towards glycolysis. It is known that parasympathetic activation inhibits the activation and release of inflammatory cytokines from macrophages in the spleen, thereby limiting excessive inflammatory responses. We hypothesize that acetylcholine, the main neurotransmitter of the parasympathetic nervous system, reduces the glycolytic metabolic activity of LPS-activated monocytes via α7-nicotinic acetylcholine receptors. In our master's thesis, we used experiments with the Seahorse XFe24 analyzer to test whether incubation of activated monocytes with the non-selective cholinergic agent acetylcholine inhibits their glycolytic activity. Using specific cholinergic antagonists, we investigated whether this inhibition is related to the effect of acetylcholine on α7-nicotinic acetylcholine receptors. Due to the presence of neutrophils in the isolated monocyte sample, we also determined their metabolic activity to evaluate their impact on the results in our monocyte isolate. Our experimental data show that acetylcholine weakly inhibited the increase in glycolytic activity of monocytes after LPS activation. This effect was only prevented by α bungarotoxin, an antagonist of α7-nicotinic acetylcholine receptors, indicating that acetylcholine inhibits the metabolic activity of activated monocytes primarily through these receptors. We did not observe a statistically significant effect of LPS activation on the mitochondrial respiration of monocytes. In experiments on the neutrophil isolate, we found that LPS significantly increased the levels of both glycolytic activity and oxidative phosphorylation, with the cholinergic influence on these metabolic changes being negligible.

Keywords:α7-nicotinic acetylcholine receptor, glycolysis, glycolytic reprogramming, cholinergic hypothesis, monocyte

Similar documents

Similar works from RUL:
Similar works from other Slovenian collections:

Back