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Literature DB >> 27617798

Combating multidrug-resistant Gram-negative bacteria with structurally nanoengineered antimicrobial peptide polymers.

Shu J Lam¹, Neil M O'Brien-Simpson², Namfon Pantarat², Adrian Sulistio¹, Edgar H H Wong¹, Yu-Yen Chen², Jason C Lenzo², James A Holden², Anton Blencowe^1,3, Eric C Reynolds², Greg G Qiao¹.

Abstract

With the recent emergence of reports on resistant Gram-negative 'superbugs', infections caused by multidrug-resistant (MDR) Gram-negative bacteria have been named as one of the most urgent global health threats due to the lack of effective and biocompatible drugs. Here, we show that a class of antimicrobial agents, termed 'structurally nanoengineered antimicrobial peptide polymers' (SNAPPs) exhibit sub-μM activity against all Gram-negative bacteria tested, including ESKAPE and colistin-resistant and MDR (CMDR) pathogens, while demonstrating low toxicity. SNAPPs are highly effective in combating CMDR Acinetobacter baumannii infections in vivo, the first example of a synthetic antimicrobial polymer with CMDR Gram-negative pathogen efficacy. Furthermore, we did not observe any resistance acquisition by A. baumannii (including the CMDR strain) to SNAPPs. Comprehensive analyses using a range of microscopy and (bio)assay techniques revealed that the antimicrobial activity of SNAPPs proceeds via a multimodal mechanism of bacterial cell death by outer membrane destabilization, unregulated ion movement across the cytoplasmic membrane and induction of the apoptotic-like death pathway, possibly accounting for why we did not observe resistance to SNAPPs in CMDR bacteria. Overall, SNAPPs show great promise as low-cost and effective antimicrobial agents and may represent a weapon in combating the growing threat of MDR Gram-negative bacteria.

Entities: Disease Species

Mesh：

Substances：

Year: 2016 PMID： 27617798 DOI： 10.1038/nmicrobiol.2016.162

Source DB: PubMed Journal: Nat Microbiol ISSN： 2058-5276 Impact factor: 17.745

47 in total

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Journal: Proc Natl Acad Sci U S A Date: 2019-05-14 Impact factor: 11.205

Combating multidrug-resistant Gram-negative bacteria with structurally nanoengineered antimicrobial peptide polymers.

1. Analysis of relative gene expression data using real-time quantitative PCR and the 2(-Delta Delta C(T)) Method.

Review 2. Designing antimicrobial peptides: form follows function.

3. Progress and challenges in implementing the research on ESKAPE pathogens.

Review 4. Bacterial programmed cell death: making sense of a paradox.

Review 5. How to address CPP and AMP translocation? Methods to detect and quantify peptide internalization in vitro and in vivo (Review).

6. The bacteria fight back.

7. Synergistic co-delivery of membrane-disrupting polymers with commercial antibiotics against highly opportunistic bacteria.

8. Monitoring antibacterial permeabilization in real time using time-resolved flow cytometry.

9. Multimerization of a Proline-Rich Antimicrobial Peptide, Chex-Arg20, Alters Its Mechanism of Interaction with the Escherichia coli Membrane.

10. Silver enhances antibiotic activity against gram-negative bacteria.

1. Arenicin-1-induced apoptosis-like response requires RecA activation and hydrogen peroxide against Escherichia coli.

2. Synthesis of polypeptides via bioinspired polymerization of in situ purified N-carboxyanhydrides.

3. Antimicrobial drugs: Multifaceted approach to multidrug resistance.

Review 4. Considerations and Caveats in Combating ESKAPE Pathogens against Nosocomial Infections.

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6. A broad-spectrum antibiotic adjuvant reverses multidrug-resistant Gram-negative pathogens.

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9. Prevention of ESKAPE pathogen biofilm formation by antimicrobial peptides WLBU2 and LL37.

10. Gold Nanoparticles with Antibiotic-Metallopolymers toward Broad-Spectrum Antibacterial Effects.