Browsing by Subject "Adenosine triphosphate"
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Item Open Access Purinergic regulation of the immune system(Nature Publishing Group, 2016) Cekic, C.; Linden, J.Cellular stress or apoptosis triggers the release of ATP, ADP and other nucleotides into the extracellular space. Extracellular nucleotides function as autocrine and paracrine signalling molecules by activating cell-surface P2 purinergic receptors that elicit pro-inflammatory immune responses. Over time, extracellular nucleotides are metabolized to adenosine, leading to reduced P2 signalling and increased signalling through anti-inflammatory adenosine (P1 purinergic) receptors. Here, we review how local purinergic signalling changes over time during tissue responses to injury or disease, and we discuss the potential of targeting purinergic signalling pathways for the immunotherapeutic treatment of ischaemia, organ transplantation, autoimmunity or cancer.Item Open Access The mechanisms of ATP - biomacromolecule interactions(Bilkent University, 2023-12) Ayvaz, CansınAdenosine triphosphate (ATP), one of the most important biomolecules of life, plays a vital role as the primary energy source within cells for essential biological functions. It has recently been discovered that ATP can also serve as a biological hydrotrope to destabilize protein aggregates and fibers. This thesis aims to investigate the recently discovered hydrotropic behavior of ATP and its interaction mechanisms with biomacromolecules, particularly poly(N-isopropylacrylamide) (PNIPAM), using a multi-experimental approach combined with molecular dynamics (MD) simulations. Adapting the bottom-up approach, the phase behavior of macromolecules is examined through phase transition and ATR-FTIR measurements. Additionally, site-specific interactions are identified with quantitative 1H-NMR spectroscopic studies, and the hydration shell structure and cluster morphologies of ATP molecules are explored through Multivariate Curve Resolution (MCR) Raman experiments. It is demonstrated that adenine and adenosine subgroups show negligible effect on the solubility of macromolecules, whereas ATP, AMP, and triphosphate exhibited purely salting-out behavior, and induced the aggregation of macromolecules. In stark contrast to the recently discovered hydrotropic behavior of ATP, no specific interactions between the macromolecule and ATP were observed in spectroscopic ATR-FTIR and 1H-NMR measurements, as well as MD simulations. Surprisingly, at elevated concentrations, self-association of ATP was observed leading to partial destabilization of larger PNIPAM aggregates to smaller ones. In the absence of ATP binding sites, interactions with random-coil-like structured macromolecules do not lead to effective hydrotropic action of ATP. Instead, they function more as stabilizers rather than solubilizing the macromolecules.