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1. Lipopolysaccharides of Brucella suis S2 Impaired the Process of Decidualization in Early Pregnancy in Mice.

2. Analysis of the Brucella suis Twin Arginine Translocation System and Its Substrates Shows That It Is Essential for Viability.

3. MapB, the Brucella suis TamB homologue, is involved in cell envelope biogenesis, cell division and virulence.

4. Interaction via the N terminus of the type IV secretion system (T4SS) protein VirB6 with VirB10 is required for VirB2 and VirB5 incorporation into T-pili and for T4SS function.

5. RegA Plays a Key Role in Oxygen-Dependent Establishment of Persistence and in Isocitrate Lyase Activity, a Critical Determinant of In vivo Brucella suis Pathogenicity.

6. Monomer-to-dimer transition of Brucella suis type IV secretion system component VirB8 induces conformational changes.

7. Structural Analysis and Inhibition of TraE from the pKM101 Type IV Secretion System.

8. Transcriptome-Wide Identification of Hfq-Associated RNAs in Brucella suis by Deep Sequencing.

9. A repA-based ELISA for discriminating cattle vaccinated with Brucella suis 2 from those naturally infected with Brucella abortus and Brucella melitensis.

10. The Brucella suis IbpA heat-shock chaperone is not required for virulence or for expression of the VirB type IV secretion system VirB8 protein.

11. Quantitative analysis of the Brucella suis proteome reveals metabolic adaptation to long-term nutrient starvation.

12. Global Rsh-dependent transcription profile of Brucella suis during stringent response unravels adaptation to nutrient starvation and cross-talk with other stress responses.

13. RegA, the regulator of the two-component system RegB/RegA of Brucella suis, is a controller of both oxidative respiration and denitrification required for chronic infection in mice.

14. Peptide nucleic acids inhibit growth of Brucella suis in pure culture and in infected murine macrophages.

15. Pathogenic brucellae replicate in human trophoblasts.

16. BtaE, an adhesin that belongs to the trimeric autotransporter family, is required for full virulence and defines a specific adhesive pole of Brucella suis.

17. The 2.5 Å structure of the enterococcus conjugation protein TraM resembles VirB8 type IV secretion proteins.

18. BmaC, a novel autotransporter of Brucella suis, is involved in bacterial adhesion to host cells.

19. Quantitative analysis of VirB8-VirB9-VirB10 interactions provides a dynamic model of type IV secretion system core complex assembly.

20. Proteomic analysis of Brucella suis under oxygen deficiency reveals flexibility in adaptive expression of various pathways.

21. Identification of VceA and VceC, two members of the VjbR regulon that are translocated into macrophages by the Brucella type IV secretion system.

22. Activity of native vs. synthetic promoters in Brucella.

23. Quantitative analysis of the intramacrophagic Brucella suis proteome reveals metabolic adaptation to late stage of cellular infection.

24. Dimerization and interactions of Brucella suis VirB8 with VirB4 and VirB10 are required for its biological activity.

25. The putative lytic transglycosylase VirB1 from Brucella suis interacts with the type IV secretion system core components VirB8, VirB9 and VirB11.

26. Functional interactions between type IV secretion systems involved in DNA transfer and virulence.

27. Requirement of MgtC for Brucella suis intramacrophage growth: a potential mechanism shared by Salmonella enterica and Mycobacterium tuberculosis for adaptation to a low-Mg2+ environment.

28. Secondary structure in the target as a confounding factor in synthetic oligomer microarray design.

29. Release of periplasmic proteins of Brucella suis upon acidic shock involves the outer membrane protein Omp25.

30. Type III secretion homologs are present in Brucella melitensis, B. ovis, and B. suis biovars 1, 2, and 3.

31. [Anti-lysozyme activity of bacteria of the genus Brucella].

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