| Literature DB >> 19799467 |
Adela Straskova1, Ivona Pavkova, Marek Link, Anna-Lena Forslund, Kerstin Kuoppa, Laila Noppa, Michal Kroca, Alena Fucikova, Jana Klimentova, Zuzana Krocova, Ake Forsberg, Jiri Stulik.
Abstract
Francisella tularensis (F. tularensis) is highly infectious for humans via aerosol route and untreated infections with the highly virulent subsp. tularensis can be fatal. Our knowledge regarding key virulence determinants has increased recently but is still somewhat limited. Surface proteins are potential virulence factors and therapeutic targets, and in this study, we decided to target three genes encoding putative membrane lipoproteins in F. tularensis LVS. One of the genes encoded a protein with high homology to the protein family of disulfide oxidoreductases DsbA. The two other genes encoded proteins with homology to the VacJ, a virulence determinant of Shigella flexneri. The gene encoding the DsbA homologue was verified to be required for survival and replication in macrophages and importantly also for in vivo virulence in the mouse infection model for tularemia. Using a combination of classical and shotgun proteome analyses, we were able to identify several proteins that accumulated in fractions enriched for membrane-associated proteins in the dsbA mutant. These proteins are substrate candidates for the DsbA disulfide oxidoreductase as well as being responsible for the virulence attenuation of the dsbA mutant.Entities:
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Year: 2009 PMID: 19799467 DOI: 10.1021/pr900570b
Source DB: PubMed Journal: J Proteome Res ISSN: 1535-3893 Impact factor: 4.466