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Harnessing the Role of Bacterial Plasma Membrane Modifications for the Development of Sustainable Membranotropic Phytotherapeutics

Gayatree Panda, Sabyasachi Dash, Santosh Kumar Sahu

2022Membranes17 citationsDOIOpen Access PDF

Abstract

Membrane-targeted molecules such as cationic antimicrobial peptides (CAMPs) are amongst the most advanced group of antibiotics used against drug-resistant bacteria due to their conserved and accessible targets. However, multi-drug-resistant bacteria alter their plasma membrane (PM) lipids, such as lipopolysaccharides (LPS) and phospholipids (PLs), to evade membrane-targeted antibiotics. Investigations reveal that in addition to LPS, the varying composition and spatiotemporal organization of PLs in the bacterial PM are currently being explored as novel drug targets. Additionally, PM proteins such as Mla complex, MPRF, Lpts, lipid II flippase, PL synthases, and PL flippases that maintain PM integrity are the most sought-after targets for development of new-generation drugs. However, most of their structural details and mechanism of action remains elusive. Exploration of the role of bacterial membrane lipidome and proteome in addition to their organization is the key to developing novel membrane-targeted antibiotics. In addition, membranotropic phytochemicals and their synthetic derivatives have gained attractiveness as popular herbal alternatives against bacterial multi-drug resistance. This review provides the current understanding on the role of bacterial PM components on multidrug resistance and their targeting with membranotropic phytochemicals.

Topics & Concepts

LipidomeFlippaseBacteriaAntibioticsDrug discoveryBacterial outer membraneDrugAntibiotic resistanceProteomeBiologyDrug resistanceLipid IIAntimicrobialChemistryMembraneBiochemistryMicrobiologyBacterial cell structureEscherichia coliPharmacologyLipidomicsPhospholipidGenePhosphatidylserineGeneticsAntimicrobial Peptides and ActivitiesAntibiotic Resistance in BacteriaBacteriophages and microbial interactions
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