publication

Impact of Antibiotic Consumption on the Acquisition of Extended-Spectrum β-Lactamase Producing Enterobacterales Carriage during the COVID-19 Crisis in French Guiana

Affiliations

1Intensive Care Unit, Cayenne General Hospital, 97306 Cayenne, French Guiana.

2Pharmacy Department, Cayenne General Hospital, 97306 Cayenne, French Guiana.

3Tropical Biome and Immunopathology CNRS UMR-9017, Inserm U 1019, Université de Guyane, 97300 Cayenne, French Guiana.

4Emergency Department, Cayenne General Hospital, 97306 Cayenne, French Guiana.

5Department of Neuro-ICU, GHU-Paris, Paris University, 75014 Paris, France.

6Clinical Investigation Center, Antilles French Guiana (CIC Inserm 1424), Cayenne General Hospital, 97306 Cayenne, French Guiana.

7Polyvalent Biology Department, Cayenne General Hospital, 97306 Cayenne, French Guiana.

8Tropical and Infectious Diseases Department, Cayenne General Hospital, 97306 Cayenne, French Guiana.

Abstract

(1) Background: During the COVID-19 outbreak, several studies showed an increased prevalence of extended-spectrum β-lactamase producing Enterobacterales (ESBL-PE) carriage in intensive care units (ICUs). Our objective was to assess the impact of antibiotic prescriptions on the acquisition of ESBL-PE in ICUs during the COVID-19 crisis. (2) Methods: We conducted an observational study between 1 April 2020, and 31 December 2021, in the medical-surgical ICU of the Cayenne General Hospital. We defined two periods: Period 1 with routine, empirical antibiotic use, and Period 2 with no systematic empiric antibiotic prescription. (3) Results: ICU-acquired ESBL-PE carriage was 22.8% during Period 1 and 9.4% during Period 2 (p = 0.005). The main isolated ESBL-PE was Klebsiella pneumoniae (84.6% in Period 1 and 58.3% in Period 2). When using a generalized linear model with a Poisson family, exposure to cefotaxime was the only factor independently associated with ESBL-PE acquisition in ICU (p = 0.002, IRR 2.59 (95% IC 1.42-4.75)). The propensity scores matching estimated the increased risk for cefotaxime use to acquire ESBL-PE carriage at 0.096 (95% CI = 0.02-0.17), p = 0.01. (4) Conclusions: Exposure to cefotaxime in patients with severe COVID-19 is strongly associated with the emergence of ESBL-PE in the context of maximal infection control measures.

Keywords: COVID-19; ESBL-PE; antibiotics; cefotaxime.