Publications by authors named "Kasper Holst Hansen"

Bacterial biofilms cause persistent infections that are difficult to treat and contribute greatly to antimicrobial resistance. However, high-resolution structural information on native bacterial biofilms remain very limited. This limitation is primarily due to methodological constraints associated with analyzing complex native samples.

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Article Synopsis
  • A high-resolution solid-state NMR study was conducted on two strains of nontuberculous mycobacteria (NTM): the non-pathogenic Mycobacterium smegmatis and the pathogenic Mycobacterium abscessus, to characterize their cell wall structures.
  • The research identified over 100 distinct carbon signals and tentatively assigned around 30 polysaccharide types, revealing detailed chemical information about NTM cell walls, including peptidoglycan and mycolic acid components.
  • Comparison through electron microscopy suggested that the cell wall of M. abscessus has a smaller, more flexible peptidoglycan layer, which may contribute to its increased pathogenicity, providing insights for future treatment strategies.
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Biofilm-protected pathogenic causes chronic infections that are difficult to treat. An essential building block of these biofilms are functional amyloid fibrils that assemble from phenol-soluble modulins (PSMs). PSMα1 cross-seeds other PSMs into cross-β amyloid folds and is therefore a key element in initiating biofilm formation.

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Functional bacterial amyloids play a crucial role in the formation of biofilms, which mediate chronic infections and contribute to antimicrobial resistance. This study focuses on the FapC amyloid fibrillar protein from Pseudomonas, a major contributor to biofilm formation. We investigate the initial steps of FapC amyloid formation and the impact of the chaperone-like protein FapA on this process.

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Phenol-soluble modulins (PSMs) are key virulence factors of , and they comprise the structural scaffold of biofilm as they self-assemble into functional amyloids. They have been shown to interact with cell membranes as they display toxicity towards human cells through cell lysis, with αPSM3 being the most cytotoxic. In addition to causing cell lysis in mammalian cells, PSMs have also been shown to interact with bacterial cell membranes through antimicrobial effects.

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