Intracellular activity and in vivo efficacy in a mouse model of septic arthritis of the novel pseudopeptide Pep16 against Staphylococcus aureus clinical isolates

Author:

Mascary Jean-Baptiste12,Bordeau Valérie1,Nicolas Irène2,Verdier Marie-Clémence3,Rocheteau Pierre2,Cattoir Vincent45ORCID

Affiliation:

1. Inserm U1230 BRM (Bacterial RNAs and Medicine), Université de Rennes , Rennes , France

2. SAS Olgram , Bréhan , France

3. CHU de Rennes, Service de Pharmacologie , Rennes , France

4. CHU de Rennes, Service de Bactériologie-Hygiène hospitalière , 2 rue Henri Le Guilloux , 35033 Rennes, France

5. CNR de la Résistance aux Antibiotiques (laboratoire associé ‘Entérocoques’), CHU de Rennes , Rennes , France

Abstract

Abstract Objectives Assessing the therapeutic potential of a novel antimicrobial pseudopeptide, Pep16, both in vitro and in vivo for the treatment of septic arthritis caused by Staphylococcus aureus. Methods Seven clinical isolates of S. aureus (two MRSA and five MSSA) were studied. MICs of Pep16 and comparators (vancomycin, teicoplanin, daptomycin and levofloxacin) were determined through the broth microdilution method. The intracellular activity of Pep16 and levofloxacin was assessed in two models of infection using non-professional (osteoblasts MG-63) or professional (macrophages THP-1) phagocytic cells. A mouse model of septic arthritis was used to evaluate the in vivo efficacy of Pep16 and vancomycin. A preliminary pharmacokinetic (PK) analysis was performed by measuring plasma concentrations using LC-MS/MS following a single subcutaneous injection of Pep16 (10 mg/kg). Results MICs of Pep16 were consistently at 8 mg/L for all clinical isolates of S. aureus (2- to 32-fold higher to those of comparators) while MBC/MIC ratios confirmed its bactericidal activity. Both Pep16 and levofloxacin (when used at 2 × MIC) significantly reduced the bacterial load of all tested isolates (two MSSA and two MRSA) within both osteoblasts and macrophages. In MSSA-infected mice, Pep16 demonstrated a significant (∼10-fold) reduction on bacterial loads in knee joints. PK analysis following a single subcutaneous administration of Pep16 revealed a gradual increase in plasma concentrations, reaching a peak of 5.6 mg/L at 12 h. Conclusions Pep16 is a promising option for the treatment of septic arthritis due to S. aureus, particularly owing to its robust intracellular activity.

Funder

BRM

CIFRE

Publisher

Oxford University Press (OUP)

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