Literature DB >> 33305953

Protein Folding Stability Changes Across the Proteome Reveal Targets of Cu Toxicity in E. coli.

Nancy Wiebelhaus1, Jacqueline M Zaengle-Barone1, Kevin K Hwang1, Katherine J Franz1, Michael C Fitzgerald1.   

Abstract

The ability of metal ionophores to induce cellular metal hyperaccumulation endows them with potent antimicrobial activity; however, the targets and mechanisms behind these outcomes are not well understood. This work describes the first utilization of proteome-wide measurements of protein folding stability in combination with protein expression level analysis to identify protein targets of copper, thereby providing new insight into ionophore-induced copper toxicity in E. coli. The protein folding stability analysis employed a one-pot protocol for pulse proteolysis (PP) in combination with a semi-tryptic peptide enrichment strategy for proteolysis procedures (STEPP) to generate stability profiles for proteins in cell lysates derived from E. coli exposed to copper with and without two ionophores, the antimicrobial agent pyrithione and its β-lactamase-activated prodrug, PcephPT. As part of this work, the above cell lysates were also subject to protein expression level analysis using conventional quantitative bottom-up proteomic methods. The protein folding stability and expression level profiles generated here enabled the effects of ionophore vs copper to be distinguished and revealed copper-driven stability changes in proteins involved in processes spanning metabolism, translation, and cell redox homeostasis. The 159 differentially stabilized proteins identified in this analysis were significantly more numerous (∼3×) than the 53 proteins identified with differential expression levels. These results illustrate the unique information that protein stability measurements can provide to decipher metal-dependent processes in drug mode of action studies.

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Year:  2020        PMID: 33305953      PMCID: PMC7984275          DOI: 10.1021/acschembio.0c00900

Source DB:  PubMed          Journal:  ACS Chem Biol        ISSN: 1554-8929            Impact factor:   5.100


  49 in total

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Review 6.  The Yin and Yang of copper during infection.

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Review 7.  Escherichia coli mechanisms of copper homeostasis in a changing environment.

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Journal:  Metallomics       Date:  2019-01-23       Impact factor: 4.526

9.  Understanding the Mechanism of Action of the Anti-Dandruff Agent Zinc Pyrithione against Malassezia restricta.

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  5 in total

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4.  Copper Induces Protein Aggregation, a Toxic Process Compensated by Molecular Chaperones.

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5.  Bioinformatic profiling identifies the glutaminase to be a potential novel cuproptosis-related biomarker for glioma.

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  5 in total

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