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Featured researches published by T J Baldwin.


Infection and Immunity | 2002

The growth response of Escherichia coli to neurotransmitters and related catecholamine drugs requires a functional enterobactin biosynthesis and uptake system

Claire L. Burton; Siri Ram Chhabra; Simon Swift; T J Baldwin; Helen Withers; Stephen J. Hill; Paul Williams

ABSTRACT The neurotransmitter norepinephrine (NE) stimulates the growth of low inocula of Escherichia coli in a minimal medium (SAPI) supplemented with serum (SAPI+serum) and induces the production of an “autoinducer” (AI) which, in turn, promotes E. coli growth in the absence of NE. Given the importance of NE, epinephrine, and their corresponding adrenergic agonists and antagonists in clinical medicine, we sought to investigate the molecular basis for these observations. Using a variety of NE precursors, metabolites, and therapeutic agents, we demonstrated that their ability to stimulate E. coli growth in SAPI+serum is dependent on the presence of a catechol (1,2-dihydroxybenzene) moiety with maximal activity requiring a two-carbon substituent incorporating a terminal primary amine. Serum contains the iron-binding glycoprotein, transferrin, and when SAPI+serum was supplemented with sufficient Fe3+ to saturate transferrin, growth inhibition was relieved. Other metal cations, including Mg2+, Ca2+, and Zn2+, had no effect. These data suggested that the stimulation of E. coli growth by NE in SAPI+serum may involve the catecholate siderophore, enterobactin, a cyclic triester of 2,3-dihydroxybenzoylserine. Consistent with this hypothesis, E. coli strains with mutations in ferrienterobactin transport (fepA or tonB) or enterobactin biosynthesis (entA) did not respond to NE. Furthermore, NE induced expression of the ferrienterobactin receptor, FepA, during growth in SAPI+serum. The enterobactin degradation product, 2,3-dihydroxybenzoylserine (DBS) was as effective as NE in stimulating the growth of E. coli and mutations in fepA or tonB abolished the DBS-dependent growth stimulation. In contrast to NE, however, DBS stimulated the growth of the entA mutant. Moreover, after growth in an iron-limited M9 medium in the absence of NE, ethyl acetate extracts of the E. coli entA+ parent but not of the entA mutant contained AI, i.e., stimulated the growth of E. coli in SAPI+serum. Taken together, these data show that when low numbers of E. coli are inoculated into SAPI+serum, NE, DBS, and related catecholamines induce the enterobactin iron uptake system. This, in turn, facilitates iron sequestration from transferrin and indicates that the AI present in NE-conditioned SAPI+serum medium is enterobactin and its DBS breakdown products.


Infection and Immunity | 2002

Role of Neisseria meningitidis luxS in Cell-to-Cell Signaling and Bacteremic Infection

Klaus Winzer; Yao-hui Sun; Andrew R. Green; Marie Delory; David Blackley; Kim R. Hardie; T J Baldwin; Christoph M. Tang

ABSTRACT Numerous pathogenic bacteria contain luxS, which is required for autoinducer-2 production. Here, we demonstrate that Neisseria meningitidis contains a functional copy of luxS that is necessary for full meningococcal virulence; strains with a luxS deletion are defective for bacteremia, a prerequisite of meningococcal pathogenesis.


Infection and Immunity | 2002

Afa, a Diffuse Adherence Fibrillar Adhesin Associated with Enteropathogenic Escherichia coli

Rogéria Keller; Juana Ordonez; Rosana R. de Oliveira; Luiz R. Trabulsi; T J Baldwin; Stuart Knutton

ABSTRACT O55 is one of the most frequent enteropathogenic Escherichia coli (EPEC) O serogroups implicated in infantile diarrhea in developing countries. Multilocus enzyme electrophoresis analysis showed that this serogroup includes two major electrophoretic types (ET), designated ET1 and ET5. ET1 corresponds to typical EPEC, whilst ET5 comprises strains with different combinations of virulence genes, including those for localized adherence (LA) and diffuse adherence (DA). Here we report that ET5 DA strains possess a DA adhesin, designated EPEC Afa. An 11.6-kb chromosomal region including the DA adhesin operon from one O55:H− ET5 EPEC strain was sequenced and found to encode a protein with 98% identity to AfaE-1, an adhesin associated with uropathogenic E. coli. Although described as an afimbrial adhesin, we show that both AfaE-1 and EPEC Afa possess fine fibrillar structures. This is the first characterization and demonstration of an Afa adhesin associated with EPEC.


Infection and Immunity | 1989

Actin accumulation at sites of bacterial adhesion to tissue culture cells:Basis of a new diagnostic test for enteropathogenic and enterohemorrhagic. Escherichia coli

Stuart Knutton; T J Baldwin; Peter H. Williams; A S McNeish


Infection and Immunity | 1991

Elevation of intracellular free calcium levels in HEp-2 cells infected with enteropathogenic Escherichia coli.

T J Baldwin; W Ward; Alastair Aitken; Stuart Knutton; Peter H. Williams


Infection and Immunity | 1993

Calcium-calmodulin dependence of actin accretion and lethality in cultured HEp-2 cells infected with enteropathogenic Escherichia coli.

T J Baldwin; M B Lee-Delaunay; Stuart Knutton; Peter H. Williams


Infection and Immunity | 1992

Enteroaggregative Escherichia coli strains secrete a heat-labile toxin antigenically related to E. coli hemolysin

T J Baldwin; Stuart Knutton; L Sellers; H A Hernandez; Alastair Aitken; Peter H. Williams


Infection and Immunity | 1996

Phosphorylation of myosin light chain at distinct sites and its association with the cytoskeleton during enteropathogenic Escherichia coli infection

H A Manjarrez-Hernandez; T J Baldwin; Peter H. Williams; Richard D. Haigh; Stuart Knutton; Alastair Aitken


Archive | 1997

Diagnostic method for measuring the ammonia content in breath

T J Baldwin; Saverio Peter Borriello; Helen M. Palmer; Christopher Geoffrey Dominic Sykesud


Fems Microbiology Letters | 1994

The 126 kDa iron-regulated protein of Listeria monocytogenes is not a transferrin binding protein

Reshma Bhatt; D. A. A. Ala'aldeen; T J Baldwin; S. Peter Borriello

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Stuart Knutton

University of Birmingham

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Kim R. Hardie

University of Nottingham

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Paul Williams

University of Nottingham

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