Literature DB >> 23115111

In vitro emergence of rifampicin resistance in Propionibacterium acnes and molecular characterization of mutations in the rpoB gene.

Ulrika Furustrand Tafin1, Andrej Trampuz, Stéphane Corvec.   

Abstract

OBJECTIVES: Activity of rifampicin against Propionibacterium acnes biofilms was recently demonstrated, but rifampicin resistance has not yet been described in this organism. We investigated the in vitro emergence of rifampicin resistance in P. acnes and characterized its molecular background.
METHODS: P. acnes ATCC 11827 was used (MIC 0.007 mg/L). The mutation rate was determined by inoculation of 10(9) cfu of P. acnes on rifampicin-containing agar plates incubated anaerobically for 7 days. Progressive emergence of resistance was studied by serial exposure to increasing concentrations of rifampicin in 72 h cycles using a low (10(6) cfu/mL) and high (10(8) cfu/mL) inoculum. The stability of resistance was determined after three subcultures of rifampicin-resistant isolates on rifampicin-free agar. For resistant mutants, the whole rpoB gene was amplified, sequenced and compared with a P. acnes reference sequence (NC006085).
RESULTS: P. acnes growth was observed on rifampicin-containing plates with mutation rates of 2 ± 1 cfu  ×  10(-9) (4096× MIC) and 12 ± 5 cfu  ×  10(-9) (4 × MIC). High-level rifampicin resistance emerged progressively after 4 (high inoculum) and 13 (low inoculum) cycles. In rifampicin-resistant isolates, the MIC remained >32 mg/L after three subcultures. Mutations were detected in clusters I (amino acids 418-444) and II (amino acids 471-486) of the rpoB gene after sequence alignment with a Staphylococcus aureus reference sequence (CAA45512). The five following substitutions were found: His-437 → Tyr, Ser-442 → Leu, Leu-444 → Ser, Ile-483 → Val and Ser-485 → Leu.
CONCLUSION: The rifampicin MIC increased from highly susceptible to highly resistant values. The resistance remained stable and was associated with mutations in the rpoB gene. To our knowledge, this is the first report of the emergence of rifampicin resistance in P. acnes.

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Year:  2012        PMID: 23115111     DOI: 10.1093/jac/dks428

Source DB:  PubMed          Journal:  J Antimicrob Chemother        ISSN: 0305-7453            Impact factor:   5.790


  11 in total

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3.  Immunoproteomic Identification of In Vivo-Produced Propionibacterium acnes Proteins in a Rabbit Biofilm Infection Model.

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4.  Finegoldia magna Isolated from Orthopedic Joint Implant-Associated Infections.

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5.  Prosthetic Shoulder Joint Infection by Cutibacterium acnes: Does Rifampin Improve Prognosis? A Retrospective, Multicenter, Observational Study.

Authors:  Helem H Vilchez; Rosa Escudero-Sanchez; Marta Fernandez-Sampedro; Oscar Murillo; Álvaro Auñón; Dolors Rodríguez-Pardo; Alfredo Jover-Sáenz; Mª Dolores Del Toro; Alicia Rico; Luis Falgueras; Julia Praena-Segovia; Laura Guío; José A Iribarren; Jaime Lora-Tamayo; Natividad Benito; Laura Morata; Antonio Ramirez; Melchor Riera
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Review 6.  Propionibacterium acnes infection after shoulder surgery.

Authors:  Benjamin K Kadler; Saurabh S Mehta; Lennard Funk
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7.  Draft Genome Sequences of Four Propionibacterium acnes Strains Isolated from Implant-Related Infections.

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8.  Rifampin-Resistant Cutibacterium (formerly Propionibacterium) namnetense Superinfection after Staphylococcus aureus Bone Infection Treatment.

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9.  Draft Genome Sequence of Highly Rifampin-Resistant Propionibacterium namnetense NTS 31307302T Isolated from a Patient with a Bone Infection.

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Journal:  Genome Announc       Date:  2016-08-11

10.  Which is the best treatment for prosthetic joint infections due to Propionibacterium acnes: need for further biofilm in vitro and experimental foreign-body in vivo studies?

Authors:  Stéphane Corvec; Guillaume G Aubin; Roger Bayston; Waheed Ashraf
Journal:  Acta Orthop       Date:  2016-04-04       Impact factor: 3.717

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