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Molecular docking-based screening of methicillin-resistant Staphylococcus aureus FEM proteins with FDA-approved drugs.


ABSTRACT: Antibiotic resistance stands as one of the most significant public health challenges in recent decades. FEM proteins are responsible for the synthesis of pentaglycine cross-bridge, a primary constituent of bacterial peptidoglycan polymer crosslinking during cell wall biosynthesis. Since they are necessary for bacterial survival and antibiotic resistance, they were considered as significant antibacterial targets. We report herein, the virtual screening and selection of FDA-approved drugs and their potent similar molecules as FEM protein inhibitors and analyzed for inhibiting affinity and their ADMET pharmacokinetic properties. This data provide a foundation for the development and optimization of structurally innovative antimicrobial drugs.

SUBMITTER: Akkiraju AG 

PROVIDER: S-EPMC10692981 | biostudies-literature | 2023

REPOSITORIES: biostudies-literature

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Molecular docking-based screening of methicillin-resistant <i>Staphylococcus aureus</i> FEM proteins with FDA-approved drugs.

Akkiraju Anjini Gayatri AG   Badugu Aishwaraya A   Das Aditi A   Sagurthi Someswar Rao SR  

Bioinformation 20231130 11


Antibiotic resistance stands as one of the most significant public health challenges in recent decades. FEM proteins are responsible for the synthesis of pentaglycine cross-bridge, a primary constituent of bacterial peptidoglycan polymer crosslinking during cell wall biosynthesis. Since they are necessary for bacterial survival and antibiotic resistance, they were considered as significant antibacterial targets. We report herein, the virtual screening and selection of FDA-approved drugs and thei  ...[more]

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