Clinical Features and Genomic Epidemiology of Bloodstream Infections Due to Enterococcal Species Other Than or in Patients With Cancer

Overview

Journal Open Forum Infect Dis

Specialty Infectious Diseases

Date 2024 Jun 5

PMID 38835498

Authors

Dierdre B Axell-House

Patrycja A Ashley

Stephanie L Egge

Truc T Tran

Claudia Pedroza

Meng Zhang

An Q Dinh

Shelby R Simar

Pranoti V Sahasrabhojane

William R Miller

Samuel A Shelburne

Blake M Hanson

Cesar A Arias

Affiliations

Soon will be listed here.

Abstract

Background: Non- non- (NFF) enterococci are a heterogeneous group of clinically pathogenic enterococci that include species with intrinsic low-level vancomycin resistance. Patients with cancer are at increased risk for bacteremia with NFF enterococci, but their clinical and molecular epidemiology have not been extensively described.

Methods: We conducted a retrospective review of all patients (n = 70) with NFF bacteremia from 2016 to 2022 at a major cancer center. The main outcomes assessed were 30-day mortality, microbiological failure (positive blood cultures for ≥4 days), and recurrence of bacteremia (positive blood culture <14 days after clearance). Whole-genome sequencing was performed on all available NFF (n = 65).

Results: Patients with hematological malignancies made up 56% of the cohort (77% had leukemia). The majority of solid malignancies (87%) were gastrointestinal in origin. The majority of infections (83%) originated from an intra-abdominal source. The most common NFF species were (50%) and (30%). Most (61%) patients received combination therapy. Bacteremia recurred in 4.3% of patients, there was a 30-day mortality of 23%, and 4.3% had microbiological failure. and isolates were genetically diverse with no spatiotemporal clustering to suggest a single strain. Frequencies of ampicillin resistance (4.3%) and daptomycin resistance (1.9%) were low. Patients with hematologic malignancy had infections with NFF enterococci that harbored more resistance genes than patients with solid malignancy ( = .005).

Conclusions: NFF bacteremia is caused by a heterogeneous population of isolates and is associated with significant mortality. Hematological malignancy is an important risk factor for infection with NFF resistant to multiple antibiotics.

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