Among enterobacteria, ESBL production is the leading cause of multidrug resistance. The first
cases of ESBL-producing Enterobacteriaceae (EBLSE) infections were described in the 1980s and
subsequently spread worldwide.
Since the turn of the century, the prevalence of EBLSE infections, particularly among E. coli
and K. pneumoniae, has increased dramatically. The emergence of multidrug-resistant enteric
bacteria (MRE) is currently a real public health problem. The European network for monitoring
antibiotic resistance in cooperation with Santé Publique France evaluated the rate of
resistance to third generation cephalosporins (C3G) among clinical strains at 10.2% for
Escherichia coli and 28.8% for Klebsiella pneumoniae. The consequences of infections with
multi-resistant enteric bacteria, mainly represented by ESBL, are currently well known, both
from an individual point of view (increased mortality and length of hospitalization) and from
a collective point of view (increased costs of care).
The current reference treatment for ESBL-producing Enterobacteriaceae infections is based on
carbapenems.
Imipenem and meropenem are the two most commonly used carbapenems in clinical practice.
Despite their similar spectrum of action, these two molecules have different pharmacokinetic
properties, notably concerning their half-life and their elimination routes (mainly urinary
for imipenem, mixed: biliary and urinary for meropenem).
Some studies have suggested that imipenem has a low impact on the digestive microbiota.
However, no studies comparing the impact of imipenem and meropenem have been conducted.
Woerther et coll. explained in their work that the digestive microbiota confers resistance to
colonization by MREs. The impact of antibiotics on the microbiota probably leads to a
breakdown of this barrier and a loss of this resistance to colonization. Moreover, each
antibiotic therapy does not impact the digestive microbiota in the same way and it seems that
antibiotics with a high activity against strict anaerobic species and/or a high biliary
elimination are the most impacting. It is therefore essential, in the era of multidrug
resistance, to look at the influence of antibiotics on the digestive microbiota and on the
emergence and carriage of MRE.
In a context where the incidence of multi-resistant bacteria is constantly increasing, it
seems relevant to conduct a study aiming at comparing the respective impact of the use of
imipenem and meropenem on the emergence of MRE and on the digestive microbiota at the
individual level. This study aims at comparing the microbiological impact (in terms of
emergence of bacterial resistance and in terms of impact on the diversity of cultivable
digestive bacteria). It will be a comparative study with matching of patients according to
age, service and previous duration of hospitalization. Indeed, the usual management of
patients with an infection requiring treatment with a carbapenem is different between the 2
participating centers. Thus, according to the usual management of patients in these 2
participating centers, patients at Avicenne Hospital are treated with meropenem and patients
at the Paris Saint-Joseph Hospital Group with imipenem, except in the case of a need for a
high daily dose (osteoarticular infection, for example) due to the neurological toxicity of
imipenem at high dosage. In the case of high-dose use, meropenem will be the preferred
molecule.