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3 research outputs found

β-Lactam Resistance Response Triggered by Inactivation of a Nonessential Penicillin-Binding Protein

Author: A Dötsch
A Zapun
AJ Schmidtke
Andreas Dötsch
Antonio Oliver
AS Ghosh
B Korat
B Moya
Bartolomé Moya
BM Meberg
C Jacobs
C Juan
C Juan
Carlos Juan
CC Sanders
CK Stover
DM Livermore
DM Livermore
F Lindberg
F Lindberg
Frederick M. Ausubel
GL Winsor
H Kishida
J Blazquez
Jesús Blázquez
JL Vincent
JV Höltje
K Poole
KF Kong
L Quénée
Laura Zamorano
LE Alksne
MB Avison
MB Avison
N Bagge
N Honore
N Honore
P Niumsup
P Stapleton
S Normark
Susanne Haussler
TY Langaee
V Plasencia
Publication venue: Public Library of Science
Publication date: 01/03/2009
Field of study

It has long been recognized that the modification of penicillin-binding proteins (PBPs) to reduce their affinity for β-lactams is an important mechanism (target modification) by which Gram-positive cocci acquire antibiotic resistance. Among Gram-negative rods (GNR), however, this mechanism has been considered unusual, and restricted to clinically irrelevant laboratory mutants for most species. Using as a model Pseudomonas aeruginosa, high up on the list of pathogens causing life-threatening infections in hospitalized patients worldwide, we show that PBPs may also play a major role in β-lactam resistance in GNR, but through a totally distinct mechanism. Through a detailed genetic investigation, including whole-genome analysis approaches, we demonstrate that high-level (clinical) β-lactam resistance in vitro, in vivo, and in the clinical setting is driven by the inactivation of the dacB-encoded nonessential PBP4, which behaves as a trap target for β-lactams. The inactivation of this PBP is shown to determine a highly efficient and complex β-lactam resistance response, triggering overproduction of the chromosomal β-lactamase AmpC and the specific activation of the CreBC (BlrAB) two-component regulator, which in turn plays a major role in resistance. These findings are a major step forward in our understanding of β-lactam resistance biology, and, more importantly, they open up new perspectives on potential antibiotic targets for the treatment of infectious diseases

Helmholtz Zentrum für Infektionsforschung Repository

Public Library of Science (PLOS)

Crossref

Directory of Open Access Journals

PubMed Central

High-Yield Production of Secreted Active Proteins by the Pseudomonas aeruginosa Type III Secretion System▿ †

Author: Derouazi M.
Epaulard O.
Guillaume M.
Marlu R.
Polack B.
Quénée L.
Toussaint B.
Publication venue: American Society for Microbiology (ASM)
Publication date: 01/06/2008
Field of study

The Escherichia coli system is the system of choice for recombinant protein production because it is possible to obtain a high protein yield in inexpensive media. The accumulation of protein in an insoluble form in inclusion bodies remains a major disadvantage. Use of the Pseudomonas aeruginosa type III secretion system can avoid this problem, allowing the production of soluble secreted proteins

Crossref

Hal - Université Grenoble Alpes

PubMed Central

Oxylipins mediate cell-to-cell communication in Pseudomonas aeruginosa

Author: A Mund
AF Oliveira
C Fuqua
CH Pohl
E Martínez
E Martínez
E Martínez
EC Pesci
FW Studier
H Towbin
HB Kaplan
J Hansen
J Lee
J Lee
JA Vizcaíno
JM Atack
JP Pearson
JR Galloway
K Papenfort
L Passador
L Quénée
LE Khmelevtsova
LR Hmelo
M Estupiñán
M Kleerebezem
M Schuster
M Whiteley
MG Kokatnur
MR Ludwig
P Williams
SE Maddocks
T Barrett
T Metsalu
V Scala
WC Fuqua
WL Ng
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref