Mechanism of AGT-Mediated Repair of dG-dC Cross-Links in the Drug Resistance to Chloroethylnitrosoureas: Molecular Docking, MD Simulation, and ONIOM (QM/MM) Investigation.
Jiaojiao WangTing RenGuohui SunNa ZhangLijiao ZhaoRugang ZhongPublished in: Journal of chemical information and modeling (2024)
Chloroethylnitrosoureas (CENUs) are important chemotherapies applied in the treatment of cancer. They exert anticancer activity by inducing DNA interstrand cross-links (ICLs) via the formation of two O 6 -alkylguanine intermediates, O 6 -chloroethylguanine ( O 6 -ClEtG) and N 1, O 6 -ethanoguanine ( N 1, O 6 -EtG). However, O 6 -alkylguanine-DNA alkyltransferase (AGT), a DNA-repair enzyme, can restore the O 6 -alkylguanine damages and thereby obstruct the formation of ICLs (dG-dC cross-link). In this study, the inhibitory mechanism of ICL formation was investigated to elucidate the drug resistance of CENUs mediated by AGT in detail. Based on the structures of the substrate-enzyme complexes obtained from docking and MD simulations, two ONIOM (QM/MM) models with different sizes of the QM region were constructed. The model with a larger QM region, which included the substrate ( O 6 -ClEtG or N 1, O 6 -EtG), a water molecule, and five residues (Tyr114, Cys145, His146, Lys165, and Glu172) in the active pocket of AGT, accurately described the repairing reaction and generated the results coinciding with the experimental outcomes. The repair process consists of two sequential steps: hydrogen transfer to form a thiolate anion on Cys145 and alkyl transfer from the O 6 site of guanine (the rate-limiting step). The repair of N 1, O 6 -EtG was more favorable than that of O 6 -ClEtG from both kinetics and thermodynamics aspects. Moreover, the comparison of the repairing process with the formation of dG-dC cross-link and the inhibition of AGT by O 6 -benzylguanine ( O 6 -BG) showed that the presence of AGT could effectively interrupt the formation of ICLs leading to drug resistance, and the inhibition of AGT by O 6 -BG that was energetically more favorable than the repair of O 6 -ClEtG could not prevent the repair of N 1, O 6 -EtG. Therefore, it is necessary to completely eliminate AGT activity before CENUs medication to enhance the chemotherapeutic effectiveness. This work provides reasonable explanations for the supposed mechanism of AGT-mediated drug resistance of CENUs and will assist in the development of novel CENU chemotherapies and their medication strategies.
Keyphrases
- molecular docking
- dna repair
- molecular dynamics
- dendritic cells
- healthcare
- systematic review
- randomized controlled trial
- dna damage
- molecular dynamics simulations
- single molecule
- circulating tumor
- type diabetes
- cell free
- adverse drug
- skeletal muscle
- squamous cell carcinoma
- emergency department
- high resolution
- young adults
- immune response
- metabolic syndrome
- nucleic acid
- high speed
- replacement therapy
- monte carlo
- circulating tumor cells
- atomic force microscopy