Advances in UDP-N-Acetylglucosamine Enolpyruvyl Transferase (MurA) Covalent Inhibition

Oliveira, Maycon Vinicius Damasceno de; Furtado, Renan Machado; Costa, Kauê Santana da; Vakal, Serhii; Lima, Anderson Henrique Lima e

doi:10.3389/fmolb.2022.889825

Cited by 7 publications

(8 citation statements)

References 53 publications

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“…The target for docking simulations was the crystallographic structure of substrate UDP-N-acetylglucosamine of enzyme 1UAE. 5 The free energies and binding modes of these most active compounds (against MurA enzyme) were studied through Schro ¨dinger software 39 on enzyme 1UAE. The active interactions of ligands 12d, 12e, and 13b as well as co-crystal UD1 are presented in Table 4 and Fig.…”

Section: Molecular Modelingmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

“…[7][8][9]11 These are attractive selective targets to develop agents against Gram-positive and Gram-negative pathogenic bacteria. 5,6,10,13 These enzymes, including Murs (MurA, MurB, MurC, MurD, MurE, MurF, and MurZ), [14][15][16] catalyse the last six steps in the formation of the final cytoplasmic peptidoglycan biosynthesis precursor uridine 5 0 -diphosphate-N-acetylmuramyl-pentapeptide (UDP-MurNAc-pentapeptide). 7,15 UDP-N-acetylglucosamine enolpyruvyl transferase (MurA) is an important enzyme involved in the first cytosolic step of bacterial cell wall synthesis.…”

Section: Introductionmentioning

confidence: 99%

“…3 PGN is one of the classic drug targets, but remains a notable target in the design of compounds with antimicrobial activity. 4,5 The inhibition against cell wall biosynthesis is a major target of antibiotics, including beta-lactam and glycopeptide antibiotics. The attractive selective targets to develop agents against Gram-positive and Gram-negative pathogenic bacteria are the enzymes participating in the biosynthesis of the bacterial cell wall, especially its essential component, i.e.…”

Section: Introductionmentioning

confidence: 99%

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Synthesis and inhibitory activity against MurA and MurZ enzymes of 4H-pyrano[2,3-d]pyrimidine–1H-1,2,3-triazole hybrid compounds having piperidine and morpholine rings

Thành

Hai

et al. 2023

New J. Chem.

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Section: Molecular Modelingmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Synthesis and inhibitory activity against MurA and MurZ enzymes of 4H-pyrano[2,3-d]pyrimidine–1H-1,2,3-triazole hybrid compounds having piperidine and morpholine rings

Thành

Hai

et al. 2023

New J. Chem.

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“…Currently, the PEP analogue fosfomycin is the only agent approved by the United States Food and Drug Administration for clinical use in the inhibition of MurA, primarily for the treatment of cystitis. Thus, it is important to highlight the increasing challenges posed by fosfomycin‐resistant microorganisms and the emergence of mutations that challenge fosfomycin effectiveness, demanding the use of covalent inhibitors of the MurA enzyme (Lima et al, 2021; Falagas et al, 2019; Xin et al, 2022; De Oliveira et al, 2022).…”

Section: Introductionmentioning

confidence: 99%

Role of UDP‐N‐acetylmuramic acid in the regulation of MurA activity revealed by molecular dynamics simulations

de Oliveira,

da Costa,

Silva

et al. 2024

Protein Science

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The peptidoglycan biosynthesis pathway plays a vital role in bacterial cells, and facilitates peptidoglycan layer formation, a fundamental structural component of the bacterial cell wall. The enzymes in this pathway are candidates for antibiotic development, as most do not have mammalian homologues. The UDP‐N‐acetylglucosamine (UNAG) enolpyruvyl transferase enzyme (MurA) in the peptidoglycan pathway cytoplasmic step is responsible for the phosphoenolpyruvate (PEP)–UNAG catalytic reaction, forming UNAG enolpyruvate and inorganic phosphate. Reportedly, UDP‐N‐acetylmuramic acid (UNAM) binds tightly to MurA forming a dormant UNAM–PEP–MurA complex and acting as a MurA feedback inhibitor. MurA inhibitors are complex, owing to competitive binding interactions with PEP, UNAM, and UNAG at the MurA active site. We used computational methods to explore UNAM and UNAG binding. UNAM showed stronger hydrogen‐bond interactions with the Arg120 and Arg91 residues, which help to stabilize the closed conformation of MurA, than UNAG. Binding free energy calculations using end‐point computational methods showed that UNAM has a higher binding affinity than UNAG, when PEP is attached to Cys115. The unbinding process, simulated using τ–random acceleration molecular dynamics, showed that UNAM has a longer relative residence time than UNAG, which is related to several complex dissociation pathways, each with multiple intermediate metastable states. This prevents the loop from opening and exposing the Arg120 residue to accommodate UNAG and potential new ligands. Moreover, we demonstrate the importance of Cys115‐linked PEP in closed‐state loop stabilization. We provide a basis for evaluating novel UNAM analogues as potential MurA inhibitors.Public significanceMurA is a critical enzyme involved in bacterial cell wall biosynthesis and is involved in antibiotic resistance development. UNAM can remain in the target protein's active site for an extended time compared to its natural substrate, UNAG. The prolonged interaction of this highly stable complex known as the ‘dormant complex’ comprises UNAM–PEP–MurA and offers insights into antibiotic development, providing potential options against drug‐resistant bacteria and advancing our understanding of microbial biology.

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Infectious and Inflammatory Microenvironment Self‐Adaptive Artificial Peroxisomes with Synergetic Co‐Ru Pair Centers for Programmed Diabetic Ulcer Therapy

Gao,

Deng,

Geng

et al. 2024

Advanced Materials

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Complex microenvironments with bacterial infection, persistent inflammation, and impaired angiogenesis are the major challenges in chronic refractory diabetic ulcers. To address this challenge, a comprehensive strategy with highly effective and integrated antimicrobial, anti‐inflammatory, and accelerated angiogenesis will offer a new pathway to the rapid healing of infected diabetic ulcers. Here, inspired by the tunable reactive oxygen species (ROS) regulation properties of natural peroxisomes, this work reports the design of infectious and inflammatory microenvironments self‐adaptive artificial peroxisomes with synergetic Co‐Ru pair centers (APCR) for programmed diabetic ulcer therapy. Benefiting from the synergistic Co and Ru atoms, the APCR can simultaneously achieve ROS production and metabolic inhibition for bacterial sterilization in the infectious microenvironment. After disinfection, the APCR can also eliminate ROS to alleviate oxidative stress in the inflammatory microenvironment and promote wound regeneration. The data demonstrate that the APCR combines highly effective antibacterial, anti‐inflammatory, and provascular regeneration capabilities, making it an efficient and safe nanomedicine for treating infectious and inflammatory diabetic foot ulcers via a programmed microenvironment self‐adaptive treatment pathway. This work expects that synthesizing artificial peroxisomes with microenvironments self‐adaptive and bifunctional enzyme‐like ROS regulation properties will provide a promising path to construct ROS catalytic materials for treating complex diabetic ulcers, trauma, or other infection‐caused diseases.

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Advances in UDP-N-Acetylglucosamine Enolpyruvyl Transferase (MurA) Covalent Inhibition

Cited by 7 publications

References 53 publications

Synthesis and inhibitory activity against MurA and MurZ enzymes of 4H-pyrano[2,3-d]pyrimidine–1H-1,2,3-triazole hybrid compounds having piperidine and morpholine rings

Synthesis and inhibitory activity against MurA and MurZ enzymes of 4H-pyrano[2,3-d]pyrimidine–1H-1,2,3-triazole hybrid compounds having piperidine and morpholine rings

Role of UDP‐N‐acetylmuramic acid in the regulation of MurA activity revealed by molecular dynamics simulations

Infectious and Inflammatory Microenvironment Self‐Adaptive Artificial Peroxisomes with Synergetic Co‐Ru Pair Centers for Programmed Diabetic Ulcer Therapy

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