Litcius/Paper detail

Interrogation of Essentiality in the Reconstructed Haemophilus influenzae Metabolic Network Identifies Lipid Metabolism Antimicrobial Targets: Preclinical Evaluation of a FabH β-Ketoacyl-ACP Synthase Inhibitor

Nahikari López-López, David San León, Sonia de Castro, Roberto Díez‐Martínez, Manuel Iglesias-Bexiga, María‐José Camarasa, Margarita Menéndez, Juan Nogales, Junkal Garmendia

2022mSystems13 citationsDOIOpen Access PDF

Abstract

Antimicrobial resistance drives the need of synergistically combined powerful computational tools and experimental work to accelerate target identification and drug development. Here, we present a high-quality metabolic model of H. influenzae and show its usefulness both as a computational framework for large experimental data set contextualization and as a tool to discover condition-independent drug targets. We focus on β-ketoacyl-acyl carrier protein synthase III FabH chemical inhibition by using a synthetic molecule with good synthetic and antimicrobial profiles that specifically binds to the active site. The mechanistic complexity of FabH inhibition may go beyond allelic variation, and the strain-dependent effect of the inhibitor tested supports the impact of metabolic context as a key factor driving bacterial cell behavior. Therefore, this study highlights the systematic metabolic evaluation of individual strains through computational frameworks to identify secondary metabolic hubs modulating drug response, which will facilitate establishing synergistic and/or more precise and robust antibacterial treatments.

Topics & Concepts

AntimicrobialComputational biologyDrug targetMetabolic networkDrug discoveryHaemophilus influenzaeBiochemistryContextualizationChemistryBiologyMicrobiologyComputer scienceAntibioticsProgramming languageInterpretation (philosophy)Microbial Metabolic Engineering and BioproductionComputational Drug Discovery MethodsProtein Structure and Dynamics
Interrogation of Essentiality in the Reconstructed Haemophilus influenzae Metabolic Network Identifies Lipid Metabolism Antimicrobial Targets: Preclinical Evaluation of a FabH β-Ketoacyl-ACP Synthase Inhibitor | Litcius