Your search keyword '"Reyrat, Jean-Marc"' showing total 7 results

1. Mycobacterium abscessus: a new antibiotic nightmare.

Author

Nessar R, Cambau E, Reyrat JM, Murray A, and Gicquel B

Subjects

Humans, Mycobacterium classification, Anti-Bacterial Agents pharmacology, Drug Resistance, Multiple, Bacterial, Mycobacterium drug effects, Mycobacterium Infections drug therapy, Mycobacterium Infections microbiology

Abstract

The intrinsic and acquired resistance of Mycobacterium abscessus to commonly used antibiotics limits the chemotherapeutic options for infections caused by these mycobacteria. Intrinsic resistance is attributed to a combination of the permeability barrier of the complex multilayer cell envelope, drug export systems, antibiotic targets with low affinity and enzymes that neutralize antibiotics in the cytoplasm. To date, acquired resistance has only been observed for aminoglycosides and macrolides, which is conferred by mutations affecting the genes encoding the antibiotic targets (rrs and rrl, respectively). Here we summarize previous and recent findings on the resistance of M. abscessus to antibiotics in light of what has been discovered for other mycobacteria. Since we can now distinguish three groups of strains belonging to M. abscessus (M. abscessus sensu stricto, Mycobacterium massiliense and Mycobacterium bolletii), studies on antibiotic susceptibility and resistance should be considered according to this new classification. This review raises the profile of this important pathogen and highlights the work needed to decipher the molecular events responsible for its extensive chemotherapeutic resistance.

Published

2012

2. Genetic analysis of new 16S rRNA mutations conferring aminoglycoside resistance in Mycobacterium abscessus.

Author

Nessar R, Reyrat JM, Murray A, and Gicquel B

Subjects

Escherichia coli, Genes, Dominant, Genes, Recessive, Genes, rRNA, Humans, Microbial Sensitivity Tests, RNA, Bacterial genetics, Selection, Genetic, Aminoglycosides pharmacology, Anti-Bacterial Agents pharmacology, Drug Resistance, Bacterial, Mycobacterium drug effects, Mycobacterium genetics, Point Mutation, RNA, Ribosomal, 16S genetics

Abstract

Objectives: We studied the development and fitness cost of 2-deoxystreptamine aminoglycoside resistance of Mycobacterium abscessus., Methods: Spontaneous 2-deoxystreptamine aminoglycoside-resistant mutants were selected and the frequency of their appearance was determined. The 3' part of the rrs gene was sequenced to characterize mutations. Additionally, we determined the MICs of aminoglycoside drugs for the different mutants obtained. The dominance/recessivity traits of the different mutations were examined and we explored the potential cost conferred by the mutations selected in vitro on the fitness of these isolates compared with the wild-type strain., Results: The in vitro mutation rate for 2-deoxystreptamine aminoglycoside resistance was ∼10(-7) mutations/cell division. In addition to the known rrs A→G substitution at position 1408 (Escherichia coli numbering), which confers kanamycin resistance (Kan(R)), three new substitutions in rrs were identified in M. abscessus Kan(R) mutants, i.e. T→A at 1406, C→T at 1409 and G→T at 1491. Heterodiploids carrying genomic mutations T→A at 1406 and A→G at 1408 with the wild-type rrs gene carried by the pNBV1 vector showed a resistant phenotype. In contrast, heterodiploids carrying genomic mutations C→T at 1409 and G→T at 1491 with the wild-type rrs gene carried by the pNBV1 vector had a susceptible phenotype. No burden on fitness was observed for the different mutations., Conclusion: Mutations in the rrs gene that confer high-level 2-deoxystreptamine aminoglycoside resistance on M. abscessus differ in their dominance/recessivity traits and have no biological cost under our experimental conditions.

Published

2011

3. The cell surface-exposed glycopeptidolipids confer a selective advantage to the smooth variants of Mycobacterium smegmatis in vitro.

Author

Kocíncová D, Winter N, Euphrasie D, Daffé M, Reyrat JM, and Etienne G

Subjects

Animals, Cell Line, Cell Membrane chemistry, Cell Membrane metabolism, Epithelial Cells immunology, Glycolipids metabolism, Glycopeptides metabolism, Macrophages immunology, Mice, Mycobacterium smegmatis metabolism, Mycobacterium smegmatis physiology, Epithelial Cells microbiology, Glycolipids chemistry, Glycopeptides chemistry, Macrophages microbiology, Mycobacterium smegmatis growth & development, Phagocytosis immunology

Abstract

The cell surface of mycobacteria is quite rich in lipids. Glycopeptidolipids, surface-exposed lipids that typify some mycobacterial species, have been associated with a phenotypic switch between rough and smooth colony morphotypes. This conversion in Mycobacterium smegmatis is correlated with the absence/presence of glycopeptidolipids on the cell surface and is due to insertion sequence mobility. Here, we show that the occurrence of a high amount of glycopeptidolipids in the smooth variant leads to lower invasion abilities and lower internalization by macrophages. We further show that the high production of glycopeptidolipids on the cell surface can confer a selective advantage to the smooth variant when grown in vitro. This higher fitness under the laboratory condition might explain the selection of smooth variants in several independent laboratories. The implications of these findings are discussed.

Published

2009

4. Lsr2 of Mycobacterium tuberculosis is a DNA-bridging protein.

Author

Chen JM, Ren H, Shaw JE, Wang YJ, Li M, Leung AS, Tran V, Berbenetz NM, Kocíncová D, Yip CM, Reyrat JM, and Liu J

Subjects

AT Rich Sequence, Bacterial Proteins chemistry, Bacterial Proteins genetics, DNA, Bacterial chemistry, DNA, Bacterial metabolism, DNA, Bacterial ultrastructure, DNA, Circular chemistry, DNA, Circular metabolism, DNA, Circular ultrastructure, DNA-Binding Proteins chemistry, DNA-Binding Proteins genetics, Microscopy, Atomic Force, Mutation, Bacterial Proteins metabolism, DNA-Binding Proteins metabolism, Mycobacterium tuberculosis genetics

Abstract

Lsr2 is a small, basic protein present in Mycobacterium and related actinomycetes. Recent studies suggest that Lsr2 is a regulatory protein involved in multiple cellular processes including cell wall biosynthesis and antibiotic resistance. However, the underlying molecular mechanisms remain unknown. In this article, we performed biochemical studies of Lsr2-DNA interactions and structure-function analysis of Lsr2. Analysis by atomic force microscopy revealed that Lsr2 has the ability to bridge distant DNA segments, suggesting that Lsr2 plays a role in the overall organization and compactness of the nucleoid. Mutational analysis identified critical residues and selection of dominant negative mutants demonstrated that both DNA binding and protein oligomerization are essential for the normal functions of Lsr2 in vivo. These results provide strong evidence that Lsr2 is a DNA bridging protein, which represents the first identification of such proteins in bacteria phylogenetically distant from the Enterobacteriaceae. DNA bridging by Lsr2 also provides a mechanism of transcriptional regulation by Lsr2.

Published

2008

5. ICDS database: interrupted CoDing sequences in prokaryotic genomes.

Author

Perrodou E, Deshayes C, Muller J, Schaeffer C, Van Dorsselaer A, Ripp R, Poch O, Reyrat JM, and Lecompte O

Subjects

Bacillus genetics, Genomics, Internet, Mycobacterium smegmatis genetics, Sequence Homology, Amino Acid, User-Computer Interface, Codon, Terminator, Databases, Genetic, Frameshift Mutation, Genome, Archaeal, Genome, Bacterial

Abstract

Unrecognized frameshifts, in-frame stop codons and sequencing errors lead to Interrupted CoDing Sequence (ICDS) that can seriously affect all subsequent steps of functional characterization, from in silico analysis to high-throughput proteomic projects. Here, we describe the Interrupted CoDing Sequence database containing ICDS detected by a similarity-based approach in 80 complete prokaryotic genomes. ICDS can be retrieved by species browsing or similarity searches via a web interface (http://www-bio3d-igbmc.u-strasbg.fr/ICDS/). The definition of each interrupted gene is provided as well as the ICDS genomic localization with the surrounding sequence. Furthermore, to facilitate the experimental characterization of ICDS, we propose optimized primers for re-sequencing purposes. The database will be regularly updated with additional data from ongoing sequenced genomes. Our strategy has been validated by three independent tests: (i) ICDS prediction on a benchmark of artificially created frameshifts, (ii) comparison of predicted ICDS and results obtained from the comparison of the two genomic sequences of Bacillus licheniformis strain ATCC 14580 and (iii) re-sequencing of 25 predicted ICDS of the recently sequenced genome of Mycobacterium smegmatis. This allows us to estimate the specificity and sensitivity (95 and 82%, respectively) of our program and the efficiency of primer determination.

Published

2006

6. The Erp protein is anchored at the surface by a carboxy-terminal hydrophobic domain and is important for cell-wall structure in Mycobacterium smegmatis.

Author

Kocíncová D, Sondén B, de Mendonça-Lima L, Gicquel B, and Reyrat JM

Subjects

Bacterial Proteins chemistry, Cell Wall chemistry, Cell Wall drug effects, Cell Wall metabolism, Detergents, Hydrophobic and Hydrophilic Interactions, Membrane Proteins chemistry, Mycobacterium smegmatis chemistry, Mycobacterium smegmatis drug effects, Protein Structure, Tertiary, Sodium Dodecyl Sulfate, Bacterial Proteins metabolism, Membrane Proteins metabolism, Mycobacterium smegmatis metabolism

Abstract

Erp (Exported Repetitive Protein), also known as P36, Pirg and Rv3810, is a member of a mycobacteria-specific family of extracellular proteins. In pathogenic species, the erp gene has been described as a virulence factor. The Erp proteins comprise three domains. The N- and C-terminal domains are similar in all mycobacterial species, while the central domain consists of a repeated module that differs considerably between species. Here we show that the Erp protein is loosely attached to the surface and that the carboxy-terminal domain, which displays hydrophobic features, anchors Erp at the surface of the bacillus. The hydrophobic region is not necessary for the complementation of the altered colony morphology of a Mycobacterium smegmatis erp- mutant but proved to be necessary to achieve resistance to detergent at wild-type levels.

Published

2004

7. Evolution of functional polymorphism in the gene coding for the Helicobacter pylori cytotoxin.

Author

Ji X, Frati F, Barone S, Pagliaccia C, Burroni D, Xu G, Rappuoli R, Reyrat JM, and Telford JL

Subjects

China epidemiology, Dyspepsia epidemiology, Dyspepsia microbiology, Genes, Bacterial, Helicobacter Infections epidemiology, Helicobacter Infections microbiology, Helicobacter pylori classification, Humans, Molecular Epidemiology, Molecular Sequence Data, Polymorphism, Genetic, Bacterial Proteins genetics, Bacterial Toxins genetics, Cytotoxins genetics, Evolution, Molecular, Helicobacter pylori genetics

Abstract

There are two functionally different alleles of the Helicobacter pylori vacA gene, which code for proteins with different in target cell specificity. The alleles (m1 and m2) differ by approximately 50% in amino acid sequence in a 300 amino acid region, the m-region, which determines specificity. An analysis of partial likelihood anomalies in a set of eight Chinese and six Western vacA genes revealed highly significant phylogenetic deviation of a region of the gene including the m-region. Phylogenetic analysis of the conserved regions of these genes failed to reveal any distinction between m1 alleles and m2 alleles, however clear cut geographic variation was observed. In the m-region, the m1 alleles also show separate clustering of Chinese and Western isolates, however the m-region of the m2 alleles has a phylogenetic structure markedly different from the rest of the gene. The data indicate that the m2 m-region was acquired and spread through the population by horizontal transfer of DNA.

Published

2002