Investigators at Institute of Microbiology zero in on legionnaire disease cell biology
2008 JAN 15 -- Current study results from the report, 'Expression of Legionella pneumophila paralogous lipid A biosynthesis genes under different growth conditions,' have been published. "Legionella pneumophila is an opportunistic pathogen that in the environment colonizes biofilms and replicates within amoebae. The bacteria employ the intracellular multiplication/defective organelle trafficking (Icm/Dot) type IV secretion system to grow intracellularly in a specific vacuole," scientists in Zurich, Switzerland report. "Using Acanthamoeba castellanii as a host cell, we have previously identified lcsC (Legionella cytotoxic suppressor), a paralogue of the lipid A disaccharide synthase lpxB, as a cytotoxic factor of L. pneumophila. A bioinformatic analysis of the genome revealed that L. pneumophila is unique in harbouring two paralogues of lpxB and two and three paralogues of the lipid A biosynthesis acyltransferases lpxA and lpxD, respectively. LcsC (lpxB1) forms a transcriptional unit with gnnA, encoding a putative UDP-GlcNAc oxidase in the biosynthetic pathway leading to 3-aminoglucosamine analogues of lipid A. LpxB2 clusters with lpxD2, lpxA2 and lpxL paralogues, encoding secondary acyltransferases. LcsC/lpxB1 and lpxB2 were found to partially complement the growth defect of an Escherichia coli lpxB conditional mutant strain, indicating that both corresponding enzymes possess lipid A disaccharide synthase activity. The two L. pneumophila lpxB paralogues are not functionally equivalent, since expression of lcsC/lpxB1 but not lpxB2 in an L. pneumophila icmG mutant is cytotoxic for A. castellanii, and LPS purified from the two strains triggers CD14-dependent tumor necrosis factor (TNF)alpha production by macrophages with a different potency. The lpxB and lpxA paralogues are expressed under various growth conditions, including broth, biofilms and in A. castellanii. While the flagellar gene flaA is mainly expressed in late stationary phase, the lpxB and lpxA paralogues are preferentially expressed in the exponential and early stationary phases. Upon exposure to hypotonic stress and nutrient deprivation, lpxA1, and to a lesser extent lcsC/lpxB1, is upregulated," wrote U. Albers and colleagues, Institute of Microbiology. The researchers concluded: "The differential regulation of lpxB or lpxA paralogues in response to changing environmental conditions might allow L. pneumophila to adapt its lipid A structure." Albers and colleagues published their study in Microbiology (Expression of Legionella pneumophila paralogous lipid A biosynthesis genes under different growth conditions. Microbiology, 2007;153(Pt 11):3817-29). For more information, contact U. Albers, ETH Zurich, Institute of Microbiology, Wolfgang-Pauli Strasse 10, HCI G405, 8093 Zurich, Switzerland. Publisher contact information for the journal Microbiology is: Society General Microbiology, Marlborough House, Basingstoke Rd., Spencers Woods, Reading RG7 1AG, Berks, England. Keywords: Switzerland, Zurich, Legionnaire Disease Cell Biology, Bioinformatics, Cell Biology, Enzyme Research, Legionella, Legionellosis, Microbiology, Opportunistic, Oxidase, Synthase. This article was prepared by World Disease Weekly editors from staff and other reports. Copyright 2008, World Disease Weekly via NewsRx.com.
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