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A multidisciplinary approach toward identification of antibiotic scaffolds for acinetobacter baumannii

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dc.contributor.author Prajapati, Jigneshkumar Dahyabhai
dc.date.accessioned 2025-12-20T04:12:50Z
dc.date.available 2025-12-20T04:12:50Z
dc.date.issued 2019-02
dc.identifier.uri https://www.cell.com/structure/fulltext/S0969-2126(18)30382-4
dc.identifier.uri http://dspace.bits-pilani.ac.in:8080/jspui/handle/123456789/20428
dc.description.abstract Research efforts to discover potential new antibiotics for Gram-negative bacteria suffer from high attrition rates due to the synergistic action of efflux systems and the limited permeability of the outer membrane (OM). One strategy to overcome the OM permeability barrier is to identify small molecules that are natural substrates for abundant OM channels and use such compounds as scaffolds for the design of efficiently permeating antibacterials. Here we present a multidisciplinary approach to identify such potential small-molecule scaffolds. Focusing on the pathogenic bacterium Acinetobacter baumannii, we use OM proteomics to identify DcaP as the most abundant channel during infection in rodents. The X-ray crystal structure of DcaP reveals a trimeric, porinlike structure and suggests that dicarboxylic acids are potential transport substrates. Electrophysiological experiments and all-atom molecular dynamics simulations confirm this notion and provide atomistic information on likely permeation pathways and energy barriers for several small molecules, including a clinically relevant b-lactamase inhibitor. en_US
dc.language.iso en en_US
dc.publisher Elsevier en_US
dc.subject Biology en_US
dc.subject Outer membrane permeability en_US
dc.subject DcaP porin channel en_US
dc.subject Small-molecule scaffolds en_US
dc.subject Antibiotic design strategy en_US
dc.title A multidisciplinary approach toward identification of antibiotic scaffolds for acinetobacter baumannii en_US
dc.type Article en_US


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