Dynamics and binding modes of free cdk2 and its two complexes with inhibitors studied by computer simulations

OTYEPKA, Michal, Zdeněk KŘÍŽ a Jaroslav KOČA. Dynamics and binding modes of free cdk2 and its two complexes with inhibitors studied by computer simulations. Journal of Biomolecular Structure & Dynamics. GUILDERLAND: ADENINE PRESS, 2002, roč. 20, č. 2, s. 141-154. ISSN 0739-1102.

Základní údaje

• Originální název: Dynamics and binding modes of free cdk2 and its two complexes with inhibitors studied by computer simulations
• Autoři: OTYEPKA, Michal (203 Česká republika), Zdeněk KŘÍŽ (203 Česká republika) a Jaroslav KOČA (203 Česká republika, garant).
• Vydání: Journal of Biomolecular Structure & Dynamics, GUILDERLAND, ADENINE PRESS, 2002, 0739-1102.

Další údaje

• Originální jazyk: angličtina
• Typ výsledku: Článek v odborném periodiku
• Obor: 10610 Biophysics
• Stát vydavatele: Spojené státy
• Utajení: není předmětem státního či obchodního tajemství
• Impakt faktor: Impact factor: 1.009
• Kód RIV: RIV/00216224:14310/02:00006680
• Organizační jednotka: Přírodovědecká fakulta
• UT WoS: 000179043800001
• Klíčová slova anglicky: cyclin dependent kinase; drug design; inhibitors; molecular dynamics; roscovitine
• Štítky: Cyclin dependent kinase, drug design, inhibitors, molecular dynamics, roscovitine

Anotace

This article presents a molecular dynamics (MD) study of the cdk2 enzyme and its two complexes with the inhibitors isopentenyladenine and roscovitine using the Cornell et at. force field from the AMBER software package. The results show that inserting an inhibitor into the enzyme active site does not considerably change enzyme structure but it seemingly changes the distribution of internal motions. The inhibitor causes differences in the domain motions in free cdk2 and in its complexes. It was found out that repulsion of roscovitine N9 substituent causes conformational change on Lys 33 side chain. Isopentenyladenine forms with Lys 33 side chain terminal amino group a hydrogen bond. It implies that the cavity, where N9 substituent of roscovitine is buried, can adopt larger substituent due to Lys 33 side chain flexibility. The composition of electrostatic and van der Waals interactions between the inhibitor and the enzyme were also calculated along both cdk2/inhibitor MD trajectories together with MM-PB/GBSA analysis. These results show that isopentenyladenine-like inhibitors could be more effective after modifications leading to an increase in their van der Waals contact with the enzyme. We suggest that a way leading to better inhibitors occupying isopentenyladenine binding mode could be: to keep N9 and N7 purine positions free, to keep 3,3-dimethylallylamino group at C6 position, and to add, e.g., benzylamino group at C2 position. The results support the idea that the isopentenyl adenine binding mode can be used for cdk2 inhibitors design and that all possibilities to improve this binding mode were not uncovered yet.

Návaznosti

• GV201/98/K041, projekt VaV: Název: HCILAB - Laboratoř interakcí člověka s počítačem

Investor: Grantová agentura ČR, HCILAB - Laboratoř interakcí člověka s počítačem