Publications by authors named "David S Weiss"

The immunologic consequences of using bactericidal versus bacteriostatic antibiotic treatments are unclear. We observed a bacteriostatic (growth halting) treatment was more protective than a bactericidal (bacteria killing) treatment in a murine peritonitis model. To understand this unexpected difference, we compared macrophage responses to bactericidal treated bacteria or bacteriostatic treated bacteria.

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  • Contact-dependent hemolysins are key virulence factors in certain human pathogens, like gonococci, with phospholipase A being a notable outer membrane protein that can lyse human red blood cells over three days.
  • Mutations in the phospholipase A gene significantly impair the bacteria's ability to survive in human immune cells, indicating its critical role in pathogenesis.
  • The inability of phospholipase A mutants to effectively lyse host cells underscores its importance for gonococcal survival and evasion of the host's immune response.
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The cell division protein FtsN was proposed to coordinate septal peptidoglycan (sPG) synthesis and degradation to ensure robust cell wall constriction without lethal lesions. Although the precise mechanism remains unclear, previous work highlights the importance of two FtsN domains: the E domain, which interacts with and activates the sPG synthesis complex FtsWIQLB, and the SPOR domain, which binds to denuded glycan (dnG) strands, key intermediates in sPG degradation. Here, we used single-molecule tracking of FtsN and FtsW (a proxy for the sPG synthesis complex FtsWIQLB) to investigate how FtsN coordinates the two opposing processes.

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  • Most bacteria have a cell wall made of peptidoglycan, which consists of glycan strands linked by peptide cross-links, primarily classified as 4-3 and 3-3 based on their amino acid composition.
  • The majority of bacteria rely on 4-3 cross-links for survival, but in a specific intestinal pathogen, 3-3 cross-links are essential, making L,D-transpeptidases (LDTs) crucial for its viability.
  • This study identifies a new family of PG cross-linking enzymes, reveals the function of VanW domains, and highlights the potential of targeting LDTs for antibiotic development against this pathogen.
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  • * The study reveals that a phenomenon called heteroresistance, where a small population of fungal cells can resist treatment, is responsible for these infections and is prevalent among clinical isolates from different regions.
  • * To address this, researchers developed a machine learning tool that can quickly identify heteroresistance in C. parapsilosis using genomic data, which could enhance diagnosis and treatment strategies for affected patients.
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Background: Piperacillin/tazobactam is a β-lactam/β-lactamase inhibitor combination with a broad spectrum of activity that is often used as empirical and/or targeted therapy among hospitalized patients. Heteroresistance (HR) is a form of antibiotic resistance in which a minority population of resistant cells coexists with a majority susceptible population that has been found to be a cause of antibiotic treatment failure in murine models.

Objectives: To determine the prevalence of HR and mechanisms of HR to piperacillin/tazobactam among bloodstream infection (BSI) isolates.

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Antibiotics are considered one of the most important contributions to clinical medicine in the last century. Due to the use and overuse of these drugs, there have been increasing frequencies of infections with resistant pathogens. One form of resistance, heteroresistance, is particularly problematic; pathogens appear sensitive to a drug by common susceptibility tests.

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  • The text discusses a specific bacterium known for causing antibiotic-associated diarrhea, which strengthens its cell wall using 3-3 crosslinks created by L,D-transpeptidases (LDTs), unlike most bacteria that use 4-3 crosslinks.
  • Researchers found that 3-3 crosslinking is vital for the survival of this bacterium and discovered a new type of LDT that uses a VanW domain to facilitate this process.
  • The study suggests that targeting LDTs could lead to new antibiotics that effectively kill this bacterium while preserving the beneficial intestinal bacteria.
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Unlabelled: Daptomycin is a cyclic lipopeptide antibiotic used to treat infections caused by some Gram-positive bacteria. Daptomycin disrupts synthesis of the peptidoglycan (PG) cell wall by inserting into the cytoplasmic membrane and binding multiple forms of the undecaprenyl carrier lipid required for PG synthesis. Membrane insertion requires phosphatidylglycerol, so studies of daptomycin can provide insight into assembly and maintenance of the cytoplasmic membrane.

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Multidrug-resistant organism (MDRO) colonization is a fundamental challenge in antimicrobial resistance. Limited studies have shown that fecal microbiota transplantation (FMT) can reduce MDRO colonization, but its mechanisms are poorly understood. We conducted a randomized, controlled trial of FMT for MDRO decolonization in renal transplant recipients called PREMIX (NCT02922816).

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  • Antibiotics have been crucial in medicine over the last century, but their overuse is leading to more infections with drug-resistant pathogens, particularly heteroresistance.
  • Two mathematical models were developed to examine how heteroresistance emerges and changes during and after antibiotic treatment, one being progressive (where resistance increases in stages) and the other non-progressive (where different resistance levels arise directly from susceptible populations).
  • The findings suggest that current testing methods for identifying heteroresistance are inadequate and propose that future definitions should include how quickly resistant bacteria can revert to being susceptible.
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The gut-brain axis, a bidirectional signaling network between the intestine and the central nervous system, is crucial to the regulation of host physiology and inflammation. Recent advances suggest a strong correlation between gut dysbiosis and neurological diseases, however, relatively little is known about how gut bacteria impact the brain. Here, we reveal that gut commensal bacteria can translocate directly to the brain when mice are fed an altered diet that causes dysbiosis and intestinal permeability, and that this also occurs without diet alteration in distinct murine models of neurological disease.

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Antibiotic resistance causes 1.27 million global deaths annually and is predicted to worsen. Heteroresistance is a form of resistance in which only a minor and unstable subpopulation of cells of a bacterial isolate are resistant to a given antibiotic, and are therefore often undetected by clinical diagnostics.

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  • Colistin heteroresistance (HR) in bacteria involves different subpopulations with varying levels of resistance, mainly found in carbapenem-resistant Acinetobacter baumannii.
  • In a study of 173 clinical isolates, a high prevalence of HR (67.1%) was observed, and many strains (80.2%) evolved into full resistance after exposure to colistin.
  • The study reveals that HR strains are linked to worse clinical outcomes, particularly higher 14-day mortality rates in patients with bacteremia, highlighting a public health concern in healthcare settings.
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Hydrodynamics accurately describe relativistic heavy-ion collision experiments well before local thermal equilibrium is established. This unexpectedly rapid onset of hydrodynamics-which takes place on the fastest available timescale-is called hydrodynamization. It occurs when an interacting quantum system is quenched with an energy density that is much greater than its ground-state energy density.

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Phenotypic heterogeneity is an important mechanism for regulating bacterial virulence, where a single regulatory switch is typically activated to generate virulent and avirulent subpopulations. The opportunistic pathogen can transition at high frequency between virulent opaque (VIR-O) and avirulent translucent subpopulations, distinguished by cells that form opaque or translucent colonies. We demonstrate that expression of 11 TetR-type transcriptional regulators (TTTRs) can drive cells from the VIR-O opaque subpopulation to cells that form translucent colonies.

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FtsN plays an essential role in promoting the inward synthesis of septal peptidoglycan (sPG) by the FtsWI complex during bacterial cell division. How it achieves this role is unclear. Here we use single-molecule tracking to investigate FtsN's dynamics during sPG synthesis in E.

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Bacterial SPOR domains target proteins to the divisome by binding septal peptidoglycan (PG) at sites where cell wall amidases have removed stem peptides. These PG structures are referred to as denuded glycans. Although all characterized SPOR domains bind denuded glycans, whether there are differences in affinity is not known.

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