Scientific Reports (Mar 2022)

An animal model of limitation of gut colonization by carbapenemase-producing Klebsiella pneumoniae using rifaximin

  • Eleni Xenofontos,
  • Georgios Renieris,
  • Maria Kalogridi,
  • Dionyssia-Eirini Droggiti,
  • Kalliopi Synodinou,
  • Georgia Damoraki,
  • Panagiotis Koufargyris,
  • Labros Sabracos,
  • Evangelos J. Giamarellos-Bourboulis

DOI
https://doi.org/10.1038/s41598-022-07827-8
Journal volume & issue
Vol. 12, no. 1
pp. 1 – 9

Abstract

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Abstract Current knowledge suggests that infection by carbapenem-resistant enterobacteria is preceded by gut colonization. It is hypothesized that colonization is eradicated by non-absorbable antibiotics like rifaximin. We investigated the effect of rifaximin against carbapenem-resistant Klebsiella pneumoniae (CRKP) in vitro and in a mouse model. We studied the in vitro efficacy of rifaximin against 257 CRKP clinical isolates, 188 KPC producers and 69 OXA-48 producers, by minimum inhibitory concentration and time-kill assays. We then developed a model of gut colonization by feeding 30 C57Bl6 mice with 108 cfu of one KPC-KP isolate for 7 days; mice were pre-treated orally with saline, omeprazole or ampicillin. Then, another 60 mice with established KPC-2 gut colonization received orally for 7 consecutive days rifaximin 180 mg/kg dissolved in ethanol and 4% bile or vehicle. On days 0, 3 and 7 stool samples were collected; mice were sacrificed for determination of tissue outgrowth. At a concentration of 1000 μg/ml rifaximin inhibited 84.8% of CRKP isolates. Α 3 × log10 decrease of the starting inoculum was achieved by 100, 250 and 500 μg/ml of rifaximin after 24 h against 25, 55 and 55% of isolates. Pre-treatment with ampicillin was necessary for gut colonization by KPC-KP. Treatment with rifaximin succeeded in reducing KPC-KP load in stool and in the intestine. Rifaximin inhibits at clinically meaningful gut concentrations the majority of CRKP isolates and is efficient against gut colonization by KPC-KP.