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Characterization of adenylosuccinate synthetase from Helicobacter pylori using computational and experimental approach (CROSBI ID 692387)

Prilog sa skupa u zborniku | sažetak izlaganja sa skupa | domaća recenzija

Bubić, Ante ; Leščić Ašler, Ivana ; Bertoša, Branimir ; Luić, Marija Characterization of adenylosuccinate synthetase from Helicobacter pylori using computational and experimental approach // Simpozij studenata doktorskih studija PMF-a : knjiga sažetaka / Primožič, Ines (ur.). Zagreb, 2019. str. 39-40

Podaci o odgovornosti

Bubić, Ante ; Leščić Ašler, Ivana ; Bertoša, Branimir ; Luić, Marija

engleski

Characterization of adenylosuccinate synthetase from Helicobacter pylori using computational and experimental approach

Helicobacter pylori is a Gram-negative microaerophilic bacterium that chronically colonizes the gastric epithelium. Presence of this bacteria in humans can lead to the development of several gastrointestinal diseases ; including non- symptomatic chronic gastritis, peptic ulcer disease, gastric mucosa-associated lymphoid tissue (MALT) lymphoma, and gastric adenocarcinoma. [1] Adenylosuccinate synthetase (ADSS) is one of the key enzymes in purine salvage pathway, which catalyses condensation reaction of IMP with L- aspartate (ASP) to form adenylosuccinate by GTP hydrolysis in the presence of Mg2+ ions. Bioinformatic studies showed that H. pylori lacks the genes for de novo synthesis of purines. Consequently, the viability of H. pylori relies on salvage pathway for purine synthesis. Thus, ADSS represents a potential drug target for H. pylori infection. [2-3] Using experimental methods, such as enzyme kinetics we have successfully determined main kinetic parameters for all three substrates (ASP, GTP, IMP). Additionally, inhibition tests were done with known inhibitor (hadacidin) and with adenylosuccinate (main reaction’s product). Preliminary binding experiments were conducted for all three substrates using microscale thermophoresis, in order to obtain binding parameters. Since attempts to solve 3D-structure of ADSS using crystallography were unsuccessful as yet, homology modelling was applied to obtain 3D-model. The model was constructed using multisequence alignment based on six closely related protein structures of ADSS. Using obtained 3D model, several systems of ADSS enzyme alone, as well as in complex with different ligands, including substrates and inhibitors, were prepared for molecular dynamics (MD) simulations at the temperature of 310 K. The aim of this research is to decipher the mechanism of ADSS enzyme, with the final goal of designing new inhibitors.

adenylosuccinate synthetase ; Helicobacter pylori

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Podaci o prilogu

39-40.

2019.

objavljeno

Podaci o matičnoj publikaciji

Simpozij studenata doktorskih studija PMF-a : knjiga sažetaka

Primožič, Ines

Zagreb:

978-953-6076-49-9

Podaci o skupu

3. Simpozij studenata doktorskih studija PMF-a = 3rd Faculty of Science PhD Student Symposium

poster

22.02.2019-22.02.2019

Zagreb, Hrvatska

Povezanost rada

Kemija

Poveznice