Your search keyword '"Wunder EA"' showing total 5 results

1. Real-Time PCR Reveals Rapid Dissemination of Leptospira interrogans after Intraperitoneal and Conjunctival Inoculation of Hamsters.

Author

Wunder EA Jr, Figueira CP, Santos GR, Lourdault K, Matthias MA, Vinetz JM, Ramos E, Haake DA, Picardeau M, Dos Reis MG, and Ko AI

Subjects

Animals, Bacterial Load, Conjunctiva microbiology, Cricetinae, Disease Models, Animal, Leptospirosis diagnosis, Leptospirosis mortality, Male, Peritoneal Cavity microbiology, Real-Time Polymerase Chain Reaction, Leptospira interrogans physiology, Leptospirosis microbiology

Abstract

The pathogen Leptospira interrogans is a highly motile spirochete that causes acute and fulminant infections in humans and other accidental hosts. Hematogenous dissemination is important for infection by the pathogen but remains poorly understood because few animal model studies have used sensitive tools to quantify the bacteria. We evaluated the kinetics of leptospiral infection in Golden Syrian hamsters by a sensitive quantitative real-time PCR (TaqMan) with lipl32 as the target gene. The dissemination and bacterial burden were measured after intraperitoneal infection with a high dose (10(8)) or low dose (2.5 × 10(2)) of leptospires. We also examined the conjunctival challenge route to mimic the natural history of infection. Quantification of leptospires in perfused animals revealed that pathogens were detected in all organs of intraperitoneally infected hamsters, including the eye and brain, within 1 h after inoculation of 10(8) virulent L. interrogans bacteria. Peaks of 10(5) to 10(8) leptospires per gram or per milliliter were achieved in blood and all tissues between day 4 and day 8 after intraperitoneal inoculation of high- and low-dose challenges, respectively, coinciding with macroscopic and histological changes. The conjunctival route resulted in a delay in the time to peak organ burden in comparison to intraperitoneal infection, indicating that although infection could be established, penetration efficiency was low across this epithelial barrier. Surprisingly, infection with a large inoculum of high-passage-number attenuated L. interrogans strains resulted in dissemination to all organs in the first 4 days postinfection, albeit with a lower burden, followed by clearance from the blood and organs 7 days postinfection and survival of all animals. These results demonstrate that leptospiral dissemination and tissue invasion occur. In contrast, development of a critical level of tissue burden and pathology are dependent on the virulence of the infecting strain., (Copyright © 2016, American Society for Microbiology. All Rights Reserved.)

Published

2016

2. A putative regulatory genetic locus modulates virulence in the pathogen Leptospira interrogans.

Author

Eshghi A, Becam J, Lambert A, Sismeiro O, Dillies MA, Jagla B, Wunder EA Jr, Ko AI, Coppee JY, Goarant C, and Picardeau M

Subjects

Animals, Bacterial Proteins genetics, Base Sequence, Cell Movement physiology, Cricetinae, Disease Models, Animal, Gene Expression Regulation, Bacterial, Genetic Complementation Test, Kidney microbiology, Leptospira interrogans growth & development, Leptospira interrogans pathogenicity, Mutagenesis, Insertional, Sequence Analysis, DNA, Bacterial Proteins metabolism, Genes, Bacterial, Leptospira interrogans genetics, Virulence genetics

Abstract

Limited research has been conducted on the role of transcriptional regulators in relation to virulence in Leptospira interrogans, the etiological agent of leptospirosis. Here, we identify an L. interrogans locus that encodes a sensor protein, an anti-sigma factor antagonist, and two genes encoding proteins of unknown function. Transposon insertion into the gene encoding the sensor protein led to dampened transcription of the other 3 genes in this locus. This lb139 insertion mutant (the lb139(-) mutant) displayed attenuated virulence in the hamster model of infection and reduced motility in vitro. Whole-transcriptome analyses using RNA sequencing revealed the downregulation of 115 genes and the upregulation of 28 genes, with an overrepresentation of gene products functioning in motility and signal transduction and numerous gene products with unknown functions, predicted to be localized to the extracellular space. Another significant finding encompassed suppressed expression of the majority of the genes previously demonstrated to be upregulated at physiological osmolarity, including the sphingomyelinase C precursor Sph2 and LigB. We provide insight into a possible requirement for transcriptional regulation as it relates to leptospiral virulence and suggest various biological processes that are affected due to the loss of native expression of this genetic locus.

Published

2014

3. Inactivation of clpB in the pathogen Leptospira interrogans reduces virulence and resistance to stress conditions.

Author

Lourdault K, Cerqueira GM, Wunder EA Jr, and Picardeau M

Subjects

Animals, Bacterial Proteins genetics, Bacterial Proteins metabolism, Culture Media, Gerbillinae, Leptospira interrogans genetics, Leptospira interrogans growth & development, Mutation, Oxidative Stress genetics, Protein Isoforms genetics, Protein Isoforms metabolism, Temperature, Heat-Shock Proteins genetics, Heat-Shock Proteins metabolism, Leptospira interrogans pathogenicity, Leptospirosis microbiology, Molecular Chaperones genetics, Stress, Physiological

Abstract

Leptospira interrogans is the causative agent of leptospirosis, which is an emerging zoonotic disease. Resistance to stress conditions is largely uncharacterized for this bacterium. We therefore decided to analyze a clpB mutant that we obtained by random transposon mutagenesis. The mutant did not produce any of the two isoforms of ClpB. The clpB mutant exhibited growth defects at 30° and 37°C and in poor nutrient medium and showed increased susceptibility to oxidative stress, whereas the genetically complemented strain was restored in ClpB expression and in vitro wild-type growth. We also showed that the clpB mutant was attenuated in virulence in an animal model of acute leptospirosis. Our findings demonstrate that ClpB is involved in the general stress response. The chaperone is also necessary, either directly or indirectly, for the virulence of the pathogen L. interrogans.

Published

2011

4. Major surface protein LipL32 is not required for either acute or chronic infection with Leptospira interrogans.

Author

Murray GL, Srikram A, Hoke DE, Wunder EA Jr, Henry R, Lo M, Zhang K, Sermswan RW, Ko AI, and Adler B

Subjects

Animals, Bacterial Outer Membrane Proteins genetics, Blotting, Western, Cricetinae, Leptospira interrogans genetics, Leptospira interrogans metabolism, Leptospirosis genetics, Leptospirosis pathology, Lipoproteins genetics, Mesocricetus, Oligonucleotide Array Sequence Analysis, Polymerase Chain Reaction, Rats, Rats, Wistar, Bacterial Outer Membrane Proteins metabolism, Leptospira interrogans pathogenicity, Leptospirosis metabolism, Lipoproteins metabolism

Abstract

Leptospira interrogans is responsible for leptospirosis, a zoonosis of worldwide distribution. LipL32 is the major outer membrane protein of pathogenic leptospires, accounting for up to 75% of total outer membrane protein. In recent times LipL32 has become the focus of intense study because of its surface location, dominance in the host immune response, and conservation among pathogenic species. In this study, an lipL32 mutant was constructed in L. interrogans using transposon mutagenesis. The lipL32 mutant had normal morphology and growth rate compared to the wild type and was equally adherent to extracellular matrix. Protein composition of the cell membranes was found to be largely unaffected by the loss of LipL32, with no obvious compensatory increase in other proteins. Microarray studies found no obvious stress response or upregulation of genes that may compensate for the loss of LipL32 but did suggest an association between LipL32 and the synthesis of heme and vitamin B(12). When hamsters were inoculated by systemic and mucosal routes, the mutant caused acute severe disease manifestations that were indistinguishable from wild-type L. interrogans infection. In the rat model of chronic infection, the LipL32 mutant colonized the renal tubules as efficiently as the wild-type strain. In conclusion, this study showed that LipL32 does not play a role in either the acute or chronic models of infection. Considering the abundance and conservation of LipL32 among all pathogenic Leptospira spp. and its absence in saprophytic Leptospira, this finding is remarkable. The role of this protein in leptospiral biology and pathogenesis thus remains elusive.

Published

2009

5. Targeted mutagenesis in pathogenic Leptospira species: disruption of the LigB gene does not affect virulence in animal models of leptospirosis.

Author

Croda J, Figueira CP, Wunder EA Jr, Santos CS, Reis MG, Ko AI, and Picardeau M

Subjects

Animals, Bacterial Adhesion genetics, Blotting, Western, Cricetinae, Disease Models, Animal, Dogs, Leptospirosis pathology, Male, Mesocricetus, Microscopy, Fluorescence, Mutagenesis, Polymerase Chain Reaction, Rats, Virulence genetics, Antigens, Bacterial genetics, Genes, Bacterial, Leptospira interrogans genetics, Leptospira interrogans pathogenicity, Leptospirosis genetics

Abstract

The pathogenic mechanisms of Leptospira interrogans, the causal agent of leptospirosis, remain largely unknown. This is mainly due to the lack of tools for genetically manipulating pathogenic Leptospira species. Thus, homologous recombination between introduced DNA and the corresponding chromosomal locus has never been demonstrated for this pathogen. Leptospiral immunoglobulin-like repeat (Lig) proteins were previously identified as putative Leptospira virulence factors. In this study, a ligB mutant was constructed by allelic exchange in L. interrogans; in this mutant a spectinomycin resistance (Spc(r)) gene replaced a portion of the ligB coding sequence. Gene disruption was confirmed by PCR, immunoblot analysis, and immunofluorescence studies. The ligB mutant did not show decrease virulence compared to the wild-type strain in the hamster model of leptospirosis. In addition, inoculation of rats with the ligB mutant induced persistent colonization of the kidneys. Finally, LigB was not required to mediate bacterial adherence to cultured cells. Taken together, our data provide the first evidence of site-directed homologous recombination in pathogenic Leptospira species. Furthermore, our data suggest that LigB does not play a major role in dissemination of the pathogen in the host and in the development of acute disease manifestations or persistent renal colonization.

Published

2008