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Review article

https://doi.org/10.2478/aiht-2023-74-3717

Untying the anchor for the lipopolysaccharide: lipid A structural modification systems offer diagnostic and therapeutic options to tackle polymyxin resistance

Vanessa Rogga
Ivan Kosalec orcid id orcid.org/0000-0002-3010-1537


Full text: english pdf 3.519 Kb

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Abstract

Polymyxin antibiotics are the last resort for treating patients in intensive care units infected with multiple-resistant Gram-negative bacteria. Due to their polycationic structure, their mode of action is based on an ionic interaction with the negatively charged lipid A portion of the lipopolysaccharide (LPS). The most prevalent polymyxin resistance mechanisms involve covalent modifications of lipid A: addition of the cationic sugar 4-amino-L-arabinose (L-Ara4N) and/or phosphoethanolamine (pEtN). The modified structure of lipid A has a lower net negative charge, leading to the repulsion of polymyxins and bacterial resistance to membrane disruption. Genes encoding the enzymatic systems involved in these modifications can be transferred either through chromosomes or mobile genetic elements. Therefore, new approaches to resistance diagnostics have been developed. On another note, interfering with these enzymatic systems might offer new therapeutic targets for drug discovery. This literature review focuses on diagnostic approaches based on structural changes in lipid A and on the therapeutic potential of molecules interfering with these changes.

Keywords

antimicrobial resistance; adjuvants; Gram-negative bacteria; MALDI-TOF-MS; MCR-1

Hrčak ID:

308233

URI

https://hrcak.srce.hr/308233

Publication date:

27.9.2023.

Article data in other languages: croatian

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