Affiliation:
1. Department of Molecular Biology, Princeton University, Princeton, New Jersey, USA
Abstract
ABSTRACT
Gram-negative bacteria have an outer membrane (OM) impermeable to many toxic compounds that can be further strengthened during stress. In
Enterobacteriaceae
, the envelope contains enterobacterial common antigen (ECA), a carbohydrate-derived moiety conserved throughout
Enterobacteriaceae
, the function of which is poorly understood. Previously, we identified several genes in
Escherichia coli
K-12 responsible for an RpoS-dependent decrease in envelope permeability during carbon-limited stationary phase. For one of these,
yhdP
, a gene of unknown function, deletion causes high levels of both vancomycin and detergent sensitivity, independent of growth phase. We isolated spontaneous suppressor mutants of
yhdP
with loss-of-function mutations in the ECA biosynthesis operon. ECA biosynthesis gene deletions suppressed envelope permeability from
yhdP
deletion independently of envelope stress responses and interactions with other biosynthesis pathways, demonstrating suppression is caused directly by removing ECA. Furthermore,
yhdP
deletion changed cellular ECA levels and
yhdP
was found to co-occur phylogenetically with the ECA biosynthesis operon. Cells make three forms of ECA: ECA lipopolysaccharide (LPS), an ECA chain linked to LPS core; ECA phosphatidylglycerol, a surface-exposed ECA chain linked to phosphatidylglycerol; and cyclic ECA, a cyclized soluble ECA molecule found in the periplasm. We determined that the suppression of envelope permeability with
yhdP
deletion is caused specifically by the loss of cyclic ECA, despite lowered levels of this molecule found with
yhdP
deletion. Furthermore, removing cyclic ECA from wild-type cells also caused changes to OM permeability. Our data demonstrate cyclic ECA acts to maintain the OM permeability barrier in a manner controlled by YhdP.
IMPORTANCE
Enterobacterial common antigen (ECA) is a surface antigen made by all members of
Enterobacteriaceae
, including many clinically relevant genera (e.g.,
Escherichia
,
Klebsiella
,
Yersinia
). Although this surface-exposed molecule is conserved throughout
Enterobacteriaceae
, very few functions have been ascribed to it. Here, we have determined that the periplasmic form of ECA, cyclic ECA, plays a role in maintaining the outer membrane permeability barrier. This activity is controlled by a protein of unknown function, YhdP, and deletion of
yhdP
damages the OM permeability barrier in a cyclic ECA-dependent manner, allowing harmful molecules such as antibiotics into the cell. This role in maintenance of the envelope permeability barrier is the first time a phenotype has been described for cyclic ECA. As the Gram-negative envelope is generally impermeable to antibiotics, understanding the mechanisms through which the barrier is maintained and antibiotics are excluded may lead to improved antibiotic delivery.
Funder
HHS | NIH | National Institute of General Medical Sciences
Publisher
American Society for Microbiology