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. 2022 Nov 17;12(1):107.
doi: 10.1186/s13613-022-01079-5.

Clinical outcome of wild-type AmpC-producing Enterobacterales infection in critically ill patients treated with β-lactams: a prospective multicenter study

Roman Mounier  1   2   3   4 Ronan Le Guen  5 Paul-Louis Woerther  5 Mathieu Nacher  6 Clément Bonnefon  7 Nicolas Mongardon  8   9   10 Olivier Langeron  8 Eric Levesque  8   9 Séverine Couffin  11 Stéphanie Houcke  12 Michel Wolff  7 Ariane Roujansky  12 Caroline Schimpf  7 Armand Mekontso Dessap  13 Fabrice Cook  12 Keyvan Razazi  13 Hatem Kallel  12   14
Affiliations

Clinical outcome of wild-type AmpC-producing Enterobacterales infection in critically ill patients treated with β-lactams: a prospective multicenter study

Roman Mounier et al. Ann Intensive Care. .

Abstract

Background: β-lactams are the main antibiotics used against wild-type AmpC-producing Enterobacterales (wtAE). However, they may fail or select AmpC-overproducing mutants. Our aim was to assess factors associated with clinical failure of β-lactams in the treatment of wtAE infection.

Methods: From September 2017 to December 2020, we prospectively included all consecutive patients treated by definitive β-lactams therapy for wtAE infection in four university ICUs. Clinical failure was defined as inadequate response to antimicrobial therapy leading to death or to the switch for a broader-spectrum antibiotic.

Results: 177 patients were included and 29.4% progressed to clinical failure. E. cloacae was the most prevalent species (42.4%) and ventilator-associated pneumonia (VAP) was the most frequent wtAE infection (69.5%). Cefepime and cefotaxime were used as definitive antibiotic treatment in 42.9% and 27.7% of patients, respectively. Occurrence of AmpC-overproduction was documented in 5.6% of patients and was associated with clinical failure (p = 0.004). In multivariate analysis, VAP (p < 0.001, OR 11.58 [95% CI 3.11-43.02] and K. aerogenes (p = 0.030, OR 3.76 [95% CI 1.13-12.46]) were independently associated with clinical failure. Conversely, cefotaxime as definitive treatment was found inversely associated with the risk of clinical failure (p = 0.022, OR 0.25 [95% CI 0.08-0.82]). After inverse probability weighting, cefotaxime showed a 20% risk reduction of clinical failure (95% CI 5-35%, p = 0.007) whatever the location of infection, the SOFA score on the day of wtAE infection, or the bacterial species.

Conclusions: Clinical failure in the treatment of wtAE infections is associated with the infection site and the causal microorganism. Additionally, cefotaxime use is probably protective against clinical failure in wtAE infection.

Keywords: AmpC β-lactamases; AmpC-producing Enterobacterales; ICU; Infection; Third-generation cephalosporins.

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Conflict of interest statement

RM has been a speaker in symposium for AdvanzPharma. MW has been a speaker and participated to scientific board for Merck (MSD France) and Correvio. He has been a speaker in symposium for Gilead. RL, PLW, MN, CB, NM, OL, EL, SC, SH, AR, CS, AMD, FC, KR, and HK have no conflict.

Figures

Fig. 1
Fig. 1
Evolution of SOFA score between the two groups, failure and clinical success, from wtAE infection and as a function of time. The dotted line represents the clinical failure group and the solid line represents the clinical success group. *p < 0.02, ** ≤ 0.001
See this image and copyright information in PMC

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