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Legionella pneumophila type II protein secretion promotes virulence in the A/J mouse model of Legionnaires' disease pneumonia.
- Source :
-
Infection and immunity [Infect Immun] 2004 Jan; Vol. 72 (1), pp. 310-21. - Publication Year :
- 2004
-
Abstract
- Legionella pneumophila, the gram-negative agent of Legionnaires' disease, possesses type IV pili and a type II protein secretion (Lsp) system, both of which are dependent upon the PilD prepilin peptidase. By analyzing multiple pilD mutants and various types of Lsp mutants as well as performing trans-complementation of these mutants, we have confirmed that PilD and type II secretion genes are required for L. pneumophila infection of both amoebae and human macrophages. Based upon a complete analysis of lspDE, lspF, and lspG mutants, we found that the type II system controls the secretion of protease, RNase, lipase, phospholipase A, phospholipase C, lysophospholipase A, and tartrate-sensitive and tartrate-resistant acid phosphatase activities and influences the appearance of colonies. Examination of the developing L. pneumophila genome database indicated that the organism has two other loci (lspC and lspLM) that are predicted to promote secretion and thus a set of genes that is comparable to the type II secretion genes in other gram-negative bacteria. In contrast to lsp mutants, L. pneumophila pilus mutants lacking either the PilQ secretin, the PspA pseudopilin, or pilin were not defective for colonial growth, secreted activities, or intracellular replication. L. pneumophila dot/icm mutants were also not impaired for type II-dependent exoenzymes. Upon intratracheal inoculation into A/J mice, lspDE, lspF, and pilD mutants, but not pilus mutants, exhibited a reduced ability to grow in the lung, as measured by competition assays. The lspF mutant was also defective in an in vivo kinetic assay. Examination of infected mouse sera revealed that type II secreted proteins are expressed in vivo. Thus, the L. pneumophila Lsp system is a virulence factor and the only type II secretion system linked to intracellular infection.
- Subjects :
- Animals
Bacterial Proteins genetics
Disease Models, Animal
Endopeptidases genetics
Female
Fimbriae Proteins genetics
Fimbriae, Bacterial metabolism
Hartmannella microbiology
Humans
Legionella pneumophila genetics
Legionella pneumophila metabolism
Legionnaires' Disease physiopathology
Macrophages microbiology
Mice
Molecular Sequence Data
Sequence Analysis, DNA
U937 Cells
Virulence
Bacterial Proteins metabolism
Endopeptidases metabolism
Gene Expression Regulation, Bacterial
Legionella pneumophila pathogenicity
Legionnaires' Disease microbiology
Subjects
Details
- Language :
- English
- ISSN :
- 0019-9567
- Volume :
- 72
- Issue :
- 1
- Database :
- MEDLINE
- Journal :
- Infection and immunity
- Publication Type :
- Academic Journal
- Accession number :
- 14688110
- Full Text :
- https://doi.org/10.1128/IAI.72.1.310-321.2004