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PDBsum entry 2bhm
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protein Protein-protein interface(s) links
Bacterial protein PDB id
2bhm

 

 

 

 

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Contents
Protein chains
135 a.a. *
Waters ×61
* Residue conservation analysis
PDB id:
2bhm
Name: Bacterial protein
Title: Crystal structure of virb8 from brucella suis
Structure: Type iv secretion system protein virb8. Chain: a, b, c, d, e. Fragment: residues 77-239. Engineered: yes
Source: Brucella melitensis biovar suis. Brucella suis. Organism_taxid: 29461. Expressed in: escherichia coli. Expression_system_taxid: 562.
Biol. unit: Dimer (from PDB file)
Resolution:
2.40Å     R-factor:   0.246     R-free:   0.273
Authors: R.Bayliss,C.Baron,G.Waksman
Key ref:
L.Terradot et al. (2005). Structures of two core subunits of the bacterial type IV secretion system, VirB8 from Brucella suis and ComB10 from Helicobacter pylori. Proc Natl Acad Sci U S A, 102, 4596-4601. PubMed id: 15764702 DOI: 10.1073/pnas.0408927102
Date:
14-Jan-05     Release date:   16-Mar-05    
PROCHECK
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 Headers
 References

Protein chains
Pfam   ArchSchema ?
Q7CEG3  (VIRB8_BRUSU) -  Type IV secretion system protein virB8 from Brucella suis biovar 1 (strain 1330)
Seq:
Struc: 		239 a.a.
135 a.a.
Key:    PfamA domain  Secondary structure  CATH domain

 Enzyme reactions 
   Enzyme class: E.C.?
[IntEnz]   [ExPASy]   [KEGG]   [BRENDA]

 

 
DOI no: 10.1073/pnas.0408927102 Proc Natl Acad Sci U S A 102:4596-4601 (2005)
PubMed id: 15764702  
 
 
Structures of two core subunits of the bacterial type IV secretion system, VirB8 from Brucella suis and ComB10 from Helicobacter pylori.
L.Terradot, R.Bayliss, C.Oomen, G.A.Leonard, C.Baron, G.Waksman.
 
  ABSTRACT  
 
Type IV secretion systems (T4SSs) are commonly used secretion machineries in Gram-negative bacteria. They are used in the infection of human, animal, or plant cells and the propagation of antibiotic resistance. The T4SS apparatus spans both membranes of the bacterium and generally is composed of 12 proteins, named VirB1-11 and VirD4 after proteins of the canonical Agrobacterium tumefaciens T4SS. The periplasmic core complex of VirB8/VirB10 structurally and functionally links the cytoplasmic NTPases of the system with its outer membrane and pilus components. Here we present crystal structures of VirB8 of Brucella suis, the causative agent of brucellosis, and ComB10, a VirB10 homolog of Helicobacter pylori, the causative agent of gastric ulcers. The structures of VirB8 and ComB10 resemble known folds, albeit with novel secondary-structure modifications unique to and conserved within their respective families. Both proteins crystallized as dimers, providing detailed predictions about their self associations. These structures make a substantial contribution to the repertoire of T4SS component structures and will serve as springboards for future functional and protein-protein interaction studies by using knowledge-based site-directed and deletion mutagenesis.
 
  Selected figure(s)  
 
Figure 1.
Fig. 1. Crystal structure of B. suis pVirB8. (A) Sequence alignment of VirB8 proteins and secondary structure assignment. Amino acids of four representative homologs were aligned, from B. suis (B.sVirB8), A. tumefaciens (A.tVirB8, 21% identical to B.sVirB8), H. pylori Cag [H.pCag10 (HP0530, 14% identity], and ComB [H.pComB8 (HP0030), 18% identity] systems (38). Strictly conserved, strongly conserved, and conserved residues are marked in red, magenta, and light pink, respectively. The modeled region (residues 97-188 and 191-234) is shown as a gray line above the sequence for nonregular structure or as cyan boxes and yellow arrows for -helices and -strands, respectively. Green dots mark residues involved in VirB8 self association. Purple stars indicate residues mutated in previous functional studies. (B) Overall fold of pVirB8. Secondary structure representation and labels are as in A. (C) Structure of NTF2, most similar fold to pVirB8. Boxes mark the two major points of difference between the NTF2 and pVirB8 fold, the addition of 4 (blue box), and the loss of two strands (red box). (D) Surface representation of VirB8 coloring side chains by degree of conservation, as shown in A. Orientation is as in B. (E) pVirB8 dimer. Both monomers are shown in ribbon representation with the monomer on the left shown as in B but turned 90° clockwise. The other monomer is in gray. Ile-112 and Tyr-120 are shown in stick representation and colored in magenta and green, respectively. (F) Top-down view of pVirB8 dimer showing side chains involved in interface as marked in A. For clarity, one pVirB8 chain is colored gray, and the other is colored as in B. Residues at the interface are in stick representation, color-coded in green, and labeled. The figure was produced by using PYMOL, http://pymol.sourceforge.net. 		Figure 3.
Fig. 3. Dimer interface and flexible helical region of pComB10. (A) Crystallographic dimer of pComB10. One monomer (in same orientation as Fig. 2B) is shown as a surface representation of charge potential. The second monomer is shown as a ribbon. 1, 4, 6a, and 6b are shown. (B) Superposition of three representative chains shows conformational flexibility in the protruding helical region. B was produced by using PYMOL, and A was produced by using GRASP (39).
 
  Figures were selected by an automated process.  

Literature references that cite this PDB file's key reference

  PubMed id Reference
  21352491 L.Terradot, and G.Waksman (2011).
Architecture of the Helicobacter pylori Cag-type IV secretion system.
  FEBS J, 278, 1213-1222.  
20070257 A.T.Rêgo, V.Chandran, and G.Waksman (2010).
Two-step and one-step secretion mechanisms in Gram-negative bacteria: contrasting the type IV secretion system and the chaperone-usher pathway of pilus biogenesis.
  Biochem J, 425, 475-488.  
20621482 G.Waksman, and R.Fronzes (2010).
Molecular architecture of bacterial type IV secretion systems.
  Trends Biochem Sci, 35, 691-698.  
20642798 K.Wallden, A.Rivera-Calzada, and G.Waksman (2010).
Type IV secretion systems: versatility and diversity in function.
  Cell Microbiol, 12, 1203-1212.  
19946141 C.E.Alvarez-Martinez, and P.J.Christie (2009).
Biological diversity of prokaryotic type IV secretion systems.
  Microbiol Mol Biol Rev, 73, 775-808.  
19251859 G.Bourg, R.Sube, D.O'Callaghan, and G.Patey (2009).
Interactions between Brucella suis VirB8 and its homolog TraJ from the plasmid pSB102 underline the dynamic nature of type IV secretion systems.
  J Bacteriol, 191, 2985-2992.  
19279686 J.J.Gillespie, N.C.Ammerman, S.M.Dreher-Lesnick, M.S.Rahman, M.J.Worley, J.C.Setubal, B.S.Sobral, and A.F.Azad (2009).
An anomalous type IV secretion system in Rickettsia is evolutionarily conserved.
  PLoS ONE, 4, e4833.  
19508287 M.Llosa, C.Roy, and C.Dehio (2009).
Bacterial type IV secretion systems in human disease.
  Mol Microbiol, 73, 141-151.  
20033031 P.J.Christie (2009).
Structural biology: Translocation chamber's secrets.
  Nature, 462, 992-994.  
19131631 R.Fronzes, E.Schäfer, L.Wang, H.R.Saibil, E.V.Orlova, and G.Waksman (2009).
Structure of a type IV secretion system core complex.
  Science, 323, 266-268.  
19756009 R.Fronzes, P.J.Christie, and G.Waksman (2009).
The structural biology of type IV secretion systems.
  Nat Rev Microbiol, 7, 703-714.  
19946264 V.Chandran, R.Fronzes, S.Duquerroy, N.Cronin, J.Navaza, and G.Waksman (2009).
Structure of the outer membrane complex of a type IV secretion system.
  Nature, 462, 1011-1015.
PDB code: 3jqo
18084070 N.Handa, S.Kishishita, S.Morita, R.Akasaka, Z.Jin, J.Chrzas, L.Chen, Z.J.Liu, B.C.Wang, S.Sugano, A.Tanaka, T.Terada, M.Shirouzu, and S.Yokoyama (2007).
Structure of the human Tim44 C-terminal domain in complex with pentaethylene glycol: ligand-bound form.
  Acta Crystallogr D Biol Crystallogr, 63, 1225-1234.
PDB code: 2cw9
17020575 A.Economou, P.J.Christie, R.C.Fernandez, T.Palmer, G.V.Plano, and A.P.Pugsley (2006).
Secretion by numbers: Protein traffic in prokaryotes.
  Mol Microbiol, 62, 308-319.  
16648257 A.Paschos, G.Patey, D.Sivanesan, C.Gao, R.Bayliss, G.Waksman, D.O'callaghan, and C.Baron (2006).
Dimerization and interactions of Brucella suis VirB8 with VirB4 and VirB10 are required for its biological activity.
  Proc Natl Acad Sci U S A, 103, 7252-7257.  
17215876 C.Baron (2006).
VirB8: a conserved type IV secretion system assembly factor and drug target.
  Biochem Cell Biol, 84, 890-899.  
16861687 G.Patey, Z.Qi, G.Bourg, C.Baron, and D.O'Callaghan (2006).
Swapping of periplasmic domains between Brucella suis VirB8 and a pSB102 VirB8 homologue allows heterologous complementation.
  Infect Immun, 74, 4945-4949.  
16481621 S.Bailey, D.Ward, R.Middleton, J.G.Grossmann, and P.C.Zambryski (2006).
Agrobacterium tumefaciens VirB8 structure reveals potential protein-protein interaction sites.
  Proc Natl Acad Sci U S A, 103, 2582-2587.
PDB code: 2cc3
16239080 C.Baron (2005).
From bioremediation to biowarfare: on the impact and mechanism of type IV secretion systems.
  FEMS Microbiol Lett, 253, 163-170.  
16182381 J.C.Patel, O.W.Rossanese, and J.E.Galán (2005).
The functional interface between Salmonella and its host cell: opportunities for therapeutic intervention.
  Trends Pharmacol Sci, 26, 564-570.  
16153176 P.J.Christie, K.Atmakuri, V.Krishnamoorthy, S.Jakubowski, and E.Cascales (2005).
Biogenesis, architecture, and function of bacterial type IV secretion systems.
  Annu Rev Microbiol, 59, 451-485.  
The most recent references are shown first. Citation data come partly from CiteXplore and partly from an automated harvesting procedure. Note that this is likely to be only a partial list as not all journals are covered by either method. However, we are continually building up the citation data so more and more references will be included with time. Where a reference describes a PDB structure, the PDB code is shown on the right.

 

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