Rapid Phenotypic Antibiotic Susceptibility Profiling of Clinical and Blood Cultures

Overview

Journal Antibiotics (Basel)

Specialty Pharmacology

Date 2024 Mar 27

PMID 38534666

Authors

Idan Hefetz

Rita Bardenstein

Shahar Rotem

Galia Zaide

Gal Bilinsky

Ohad Shifman

Oren Zimhony

Ronit Aloni-Grinstein

Affiliations

Soon will be listed here.

Abstract

Bloodstream infections (BSI) are defined by the presence of viable bacteria or fungi, accompanied by systemic signs of infection. Choosing empirical therapy based solely on patient risk factors and prior antibiotic susceptibility test (AST) may lead to either ineffective treatment or unnecessarily broad-spectrum antibiotic exposure. In general, Clinical & Laboratory Standards Institute guideline-approved ASTs have a turnaround time of 48-72 h from sample to answer, a period that may result in a critical delay in the appropriate selection of therapy. Therefore, reducing the time required for AST is highly advantageous. We have previously shown that our novel rapid AST method, MAPt (Micro-Agar-PCR-test), accurately identifies susceptibility profiles for spiked bioterrorism agents like , and directly from whole-blood and blood culture samples, even at low bacterial levels (500 CFU/mL). This study evaluated the performance of MAPt on routine bloodstream infection (BSI), focusing on and isolates from clinical cultures, including resistant strains to some of the six tested antibiotics. Notably, MAPt yielded results exceeding 95% agreement with the standard hospital method within a significantly shorter timeframe of 6 h. These findings suggest significant potential for MAPt as a rapid and reliable BSI management tool.

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