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Data from: An In Vitro Combined Antibiotic-Antibody Treatment Eliminates Toxicity from Shiga Toxin-Producing Escherichia coli

dataset
posted on 2024-02-14, 14:42 authored by Craig Skinner, Guodong Zhang, Stephanie Patfield, Xiaohua He

Treating Shiga toxin-producing Escherichia coli (STEC) gastrointestinal infections is difficult. The utility of antibiotics for STEC treatment is controversial, since antibiotic resistance among STEC isolates is widespread and certain antibiotics dramatically increase the expression of Shiga toxins (Stxs), which are some of the most important virulence factors in STEC. Stxs contribute to life-threatening hemolytic uremic syndrome (HUS), which develops in considerable proportions of patients with STEC infections. Understanding the antibiotic resistance profiles of STEC isolates and the Stx induction potential of promising antibiotics is essential for evaluating any antibiotic treatment of STEC. In this study, 42 O157:H7 or non-O157 STEC isolates (including the “big six” serotypes) were evaluated for their resistance against 22 antibiotics by using an antibiotic array. Tigecycline inhibited the growth of all of the tested STEC isolates and also inhibited the production of Stxs (Stx2 in particular). In combination with neutralizing antibodies to Stx1 and Stx2, the tigecycline-antibody treatment fully protected Vero cells from Stx toxicity, even when the STEC bacteria and the Vero cells were cultured together. The combination of an antibiotic such as tigecycline with neutralizing antibodies presents a promising strategy for future STEC treatments.


Resources in this dataset:

  • Resource Title: Supplemental Materials.

    File Name: Web Page, url: https://aac.asm.org/content/59/9/5435/figures-only#fig-data-additional-files

    Table S1: Descriptions and characteristics of antibiotics used in this study. XLS, 35K

    Table S2: MICs of antibiotics for STEC serotypes and probiotics. XLS, 30K

    Table S3: MICs of antibiotics for individual isolates. XLS, 47K

    Table S4: Induction of Stx1 and Stx2 by selected antibiotics. XLS, 35K

Funding

USDA-ARS: 5325-42000-048-00D

History

Data contact name

He, Xiaohua

Data contact email

xiaohua.he@ars.usda.gov

Publisher

Antimicrobial Agents and Chemotherapy

Intended use

Understanding the antibiotic resistance profiles of STEC isolates and the Stx induction potential of promising antibiotics is essential for evaluating any antibiotic treatment of STEC. The combination of an antibiotic such as tigecycline with neutralizing antibodies presents a promising strategy for future STEC treatments.

Theme

  • Not specified

ISO Topic Category

  • biota
  • health

National Agricultural Library Thesaurus terms

toxicity; Shiga toxin-producing Escherichia coli; gastrointestinal system; antibiotics; antibiotic resistance; Shiga toxin; virulence; hemolytic uremic syndrome; patients; serotypes; tigecycline; neutralizing antibodies; bacteria; antibacterial properties; cultured cells; growth retardation

OMB Bureau Code

  • 005:18 - Agricultural Research Service

OMB Program Code

  • 005:040 - National Research

ARS National Program Number

  • 108

Primary article PubAg Handle

Pending citation

  • No

Public Access Level

  • Public

Preferred dataset citation

Skinner, Craig; Zhang, Guodong; Patfield, Stephanie; He, Xiaohua (2019). Data from: An In Vitro Combined Antibiotic-Antibody Treatment Eliminates Toxicity from Shiga Toxin-Producing Escherichia coli. Antimicrobial Agents and Chemotherapy.

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