Affiliation:
1. Department of Microbiology and Immunology, Northwestern University Medical School, Chicago, Illinois 60611
Abstract
ABSTRACT
Gram-negative
Legionella pneumophila
produces a siderophore (legiobactin) that promotes lung infection. We previously determined that
lbtA
and
lbtB
are required for the synthesis and secretion of legiobactin. DNA sequence and reverse transcription-PCR (RT-PCR) analyses now reveal the presence of an iron-repressed gene (
lbtU
) directly upstream of the
lbtAB
-containing operon.
In silico
analysis predicted that LbtU is an outer membrane protein consisting of a 16-stranded transmembrane β-barrel, multiple extracellular domains, and short periplasmic tails. Immunoblot analysis of cell fractions confirmed an outer membrane location for LbtU. Although replicating normally in standard media,
lbtU
mutants, like
lbtA
mutants, were impaired for growth on iron-depleted agar media. While producing typical levels of legiobactin,
lbtU
mutants were unable to use supplied legiobactin to stimulate growth on iron-depleted media and displayed an inability to take up iron. Complemented
lbtU
mutants behaved as the wild type did. The
lbtU
mutants were also impaired for infection in a legiobactin-dependent manner. Together, these data indicate that LbtU is involved in the uptake of legiobactin and, based upon its location, is most likely the
Legionella
siderophore receptor. The sequence and predicted two-dimensional (2D) and 3D structures of LbtU were distinct from those of all known siderophore receptors, which generally contain a 22-stranded β-barrel and an extended N terminus that binds TonB in order to transduce energy from the inner membrane. This observation coupled with the fact that
L. pneumophila
does not encode TonB suggests that LbtU is a new type of receptor that participates in a form of iron uptake that is mechanistically distinct from the existing paradigm.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology
Cited by
38 articles.
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