Hospital outbreak of VanA Enterococcus faecium: microbiological characterization and in vitro activity of oritavancin

Francisco Vasco-Martín; Ana Rodrigo-Moreno; Rebeca Lavilla; Alexandre Viu; Romina Romero; María Carla Iglesias; Juan Pablo Horcajada; Eduardo Padilla; María Montero; Juan Hernández

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Hospital outbreak of VanA Enterococcus faecium: microbiological characterization and in vitro activity of oritavancin

Francisco Javier Vasco-Martín

¹,

Ana Rodrigo-Moreno

^{*

1},

Rebeca Lavilla

¹,

Alexandre Viu

¹,

Romina Romero

¹,

María Carla Iglesias

²,

Juan Pablo Horcajada

²,

Eduardo Padilla

¹,

María Milagro Montero

²,

Juan José Hernández

¹ Laboratori de Referència de Catalunya, Barcelona, Spain
² Infectious Diseases Service, Hospital del Mar, Barcelona, Spain

Academic Editor: Marc Maresca

Published: 06 May 2026 by MDPI in Antibiotics 2026—Advances in Antimicrobial Action and Resistance session Antimicrobials, Antimicrobial Resistance, and One Health

Abstract:

Introduction

Vancomycin-resistant Enterococcus faecium (VREfm) is an increasing challenge in hospital settings. Although oritavancin has shown in vitro activity against some VREfm isolates, its clinical role remains uncertain because clinical breakpoints and outcome data are limited.

Objectives

To describe the epidemiological and microbiological features of a hospital outbreak caused by vanA-positive E. faecium.

To evaluate the in vitro activity of oritavancin.

Materials and methods

Bacterial identification was performed using MALDI-TOF mass spectrometry (bioMérieux VITEK® MS). The presence of vanA and related resistance determinants was assessed by next-generation sequencing (Oxford Nanopore Technologies).

Antimicrobial susceptibility was determined by broth microdilution using a commercial panel (ComASP® Oritavancin, Liofilchem).

Because EUCAST clinical breakpoints for oritavancin against E. faecium/VRE are not established, oritavancin MICs should be interpreted descriptively and compared with published MIC distributions rather than categorized as clinically susceptible or resistant.

Eight patients were identified as colonized with vanA-positive E. faecium. Cases clustered mainly in onco-hematology wards, suggesting nosocomial transmission in a high-risk population.

All isolates carried vanA and expressed high-level glycopeptide resistance, with:

Vancomycin resistance (MIC ≥ 256 mg/L)

Teicoplanin resistance (MIC ≥ 64 mg/L)

Oritavancin showed low in vitro MIC values against the outbreak isolates:

MIC range: 0.25 mg/L

Low MIC values were observed despite the presence of vanA. This finding is microbiologically relevant but should not be presented as evidence of clinical susceptibility in the absence of validated breakpoints and clinical outcomes.

Conclusions

Oritavancin demonstrated low in vitro MICs against the vanA-positive E. faecium outbreak isolates; however, these results should be considered descriptive because validated clinical breakpoints for this organism-drug combination are lacking.

Isolates showed high-level glycopeptide resistance, but retained low oritavancin MICs. Further PK/PD, synergy and clinical-outcome studies of oritavancin in VREfms to establish oritavancin as a standard therapeutic alternative for invasive infection are needed.

Keywords: VanA-positive Enterococcus faecium; Vancomycin-resistant Enterococcus (VRE); Oritavancin; Hospital outbreak

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Francisco Vasco-Martín