Analysis of CDK2 active-site hydration: A method to design new inhibitors

KŘÍŽ, Zdeněk, Michal OTYEPKA, Iveta BÁRTOVÁ a Jaroslav KOČA. Analysis of CDK2 active-site hydration: A method to design new inhibitors. Proteins: Structure, Function, and Bioinformatics. Wiley, 2004, roč. 55, č. 3, s. 258-274. ISSN 0887-3585.

Základní údaje

Originální název

Analysis of CDK2 active-site hydration: A method to design new inhibitors

Název česky

Analýza hydratace CDK2 aktivního místa

Autoři

KŘÍŽ, Zdeněk (203 Česká republika, garant), Michal OTYEPKA (203 Česká republika), Iveta BÁRTOVÁ (203 Česká republika) a Jaroslav KOČA (203 Česká republika)

Vydání

Proteins: Structure, Function, and Bioinformatics, Wiley, 2004, 0887-3585

---

Další údaje

Jazyk

angličtina

Typ výsledku

Článek v odborném periodiku

Obor

10403 Physical chemistry

Stát vydavatele

Česká republika

Utajení

není předmětem státního či obchodního tajemství

Impakt faktor

Impact factor: 4.429

Kód RIV

RIV/00216224:14310/04:00009962

Organizační jednotka

Přírodovědecká fakulta

UT WoS

000220980600007

Klíčová slova anglicky

cyclin-dependent kinase; ATP; roscovitine; isopentenyladenine; molecular dynamics; hydration of proteins; structural water molecules

Štítky

ATP, cyclin-dependent kinase, hydration of proteins, isopentenyladenine, molecular dynamics, roscovitine, structural water molecules

---

Anotace

V originále

The interactions between the protein and the solvent were analyzed, and protein regions with a high density of water molecules, as well as structural water molecules, were determined by using molecular dynamics (MD) simulations. A number of water molecules that were in contact with the protein for the whole trajectory were determined. Their interaction energies and hydrogen bonds with protein residues were analyzed. Altogether, 39, 27, 49, and 32 water molecules bound to the protein were found for trajectories of the free CDK2, CDK2/ATP, CDK2/roscovitine, and CDK2/isopentenyladenine complexes, respectively. Positions of observed water molecules were compared with X-ray crystallography data. Special attention was paid to water molecules in the active site of the enzyme, and especially to the deep pocket, where the N9 roscovitine side-chain is buried. Exchange of active-site water molecules with bulk water through the tunnel from the pocket was observed. In the CDK2/isopentenyladenine complex simulation, two water molecules that arrange interaction between the inhibitor and the enzyme via an H-bond were observed. Two stable water molecules in the trajectory of the free CDK2 were found that occupy the same position as the nitrogens N3 and N9 of the isopentenyladenine or N1 and N6 nitrogens of the adenosine triphosphate (ATP). The positions of structural water molecules were compared with the positions of substrate polar groups and crystallographic water molecules found in the Brookhaven Protein Data Bank for various CDK2 complexes. It was concluded that tracing tightly bound water molecules may substantially help in designing new inhibitors

Česky

The interactions between the protein and the solvent were analyzed, and protein regions with a high density of water molecules, as well as structural water molecules, were determined by using molecular dynamics (MD) simulations. A number of water molecules that were in contact with the protein for the whole trajectory were determined. Their interaction energies and hydrogen bonds with protein residues were analyzed. Altogether, 39, 27, 49, and 32 water molecules bound to the protein were found for trajectories of the free CDK2, CDK2/ATP, CDK2/roscovitine, and CDK2/isopentenyladenine complexes, respectively. Positions of observed water molecules were compared with X-ray crystallography data. Special attention was paid to water molecules in the active site of the enzyme, and especially to the deep pocket, where the N9 roscovitine side-chain is buried. Exchange of active-site water molecules with bulk water through the tunnel from the pocket was observed. In the CDK2/isopentenyladenine complex simulation, two water molecules that arrange interaction between the inhibitor and the enzyme via an H-bond were observed. Two stable water molecules in the trajectory of the free CDK2 were found that occupy the same position as the nitrogens N3 and N9 of the isopentenyladenine or N1 and N6 nitrogens of the adenosine triphosphate (ATP). The positions of structural water molecules were compared with the positions of substrate polar groups and crystallographic water molecules found in the Brookhaven Protein Data Bank for various CDK2 complexes. It was concluded that tracing tightly bound water molecules may substantially help in designing new inhibitors

---

Návaznosti

GV201/98/K041, projekt VaV	Název: HCILAB - Laboratoř interakcí člověka s počítačem Investor: Grantová agentura ČR, HCILAB - Laboratoř interakcí člověka s počítačem
MSM 143100005, záměr	Název: Strukturně-funkční vztahy biomolekul a jejich role v metabolismu Investor: Ministerstvo školství, mládeže a tělovýchovy ČR, Strukturně-funkční vztahy biomolekul a jejich role v metabolismu