共 45 条
QM/MM Study of the Fosfomycin Resistance Mechanism Involving FosB Enzyme
被引:4
作者:

Lima, Anderson H.
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Univ Fed Para, Inst Ciencias Exatas & Nat, Lab Planejamento & Desenvolvimento Farmacos, BR-66075110 Belem, Para, Brazil Univ Fed Para, Inst Ciencias Exatas & Nat, Lab Planejamento & Desenvolvimento Farmacos, BR-66075110 Belem, Para, Brazil

Silva, Jose Rogerio A.
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Univ Fed Para, Inst Ciencias Exatas & Nat, Lab Planejamento & Desenvolvimento Farmacos, BR-66075110 Belem, Para, Brazil Univ Fed Para, Inst Ciencias Exatas & Nat, Lab Planejamento & Desenvolvimento Farmacos, BR-66075110 Belem, Para, Brazil

Alves, Claudio Nahum
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Univ Fed Para, Inst Ciencias Exatas & Nat, Lab Planejamento & Desenvolvimento Farmacos, BR-66075110 Belem, Para, Brazil Univ Fed Para, Inst Ciencias Exatas & Nat, Lab Planejamento & Desenvolvimento Farmacos, BR-66075110 Belem, Para, Brazil

Lameira, Jeronimo
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Univ Fed Para, Inst Ciencias Exatas & Nat, Lab Planejamento & Desenvolvimento Farmacos, BR-66075110 Belem, Para, Brazil Univ Fed Para, Inst Ciencias Exatas & Nat, Lab Planejamento & Desenvolvimento Farmacos, BR-66075110 Belem, Para, Brazil
机构:
[1] Univ Fed Para, Inst Ciencias Exatas & Nat, Lab Planejamento & Desenvolvimento Farmacos, BR-66075110 Belem, Para, Brazil
来源:
关键词:
ENOLPYRUVYL TRANSFERASE MURA;
L;
D-TRANSPEPTIDASE;
CATALYTIC MECHANISM;
PROTEIN FOSA;
REGIOSELECTIVITY;
PARAMETERS;
SYNTHASE;
COMPLEX;
ORIGIN;
D O I:
10.1021/acsomega.1c00096
中图分类号:
O6 [化学];
学科分类号:
0703 ;
摘要:
Multidrug-resistant organisms contain antibiotic-modifying enzymes that facilitate resistance to a variety of antimicrobial compounds. Particularly, the fosfomycin (FOF) drug can be structurally modified by several FOF-modifying enzymes before it reaches the biological target. Among them, FosB is an enzyme that utilizes L-cysteine or bacillithiol in the presence of a divalent metal to open the epoxide ring of FOF and, consequently, inactivate the drug. Here, we have used hybrid quantum mechanics/molecular mechanics (QM/MM) and molecular dynamics (MD) simulations to explore the mechanism of the reaction involving FosB and FOF. The calculated free-energy profiles show that the cost to open the epoxide ring of FOF at the C2 atom is similar to 3.0 kcal/mol higher than that at the C1 atom. Besides, our QM/MM MD results revealed the critical role of conformation change of Cys9 and Asn50 to release the drug from the active site. Overall, the present study provides insights into the mechanism of FOF-resistant proteins.
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页码:12507 / 12512
页数:6
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