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PDBsum entry 3bx4

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protein ligands Protein-protein interface(s) links
Toxin PDB id
3bx4

 

 

 

 

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Contents
Protein chains
132 a.a. *
122 a.a. *
Ligands
SO4 ×9
GOL
Waters ×324
* Residue conservation analysis
PDB id:
3bx4
Name: Toxin
Title: Crystal structure of the snake venom toxin aggretin
Structure: Aggretin alpha chain. Chain: a, c. Aggretin beta chain. Chain: b, d
Source: Agkistrodon rhodostoma. Malayan pit viper. Secretion: venom. Secretion: venom
Resolution:
1.70Å     R-factor:   0.204     R-free:   0.236
Authors: E.Hooley,E.Papagrigoriou,A.Navdaev,A.Pandey,J.M.Clemetson, K.J.Clemetson,J.Emsley
Key ref: E.Hooley et al. (2008). The crystal structure of the platelet activator aggretin reveals a novel (alphabeta)2 dimeric structure. Biochemistry, 47, 7831-7837. PubMed id: 18597489
Date:
11-Jan-08     Release date:   26-Aug-08    
PROCHECK
Go to PROCHECK summary
 Headers
 References

Protein chains
Pfam   ArchSchema ?
Q9I841  (SLYA_CALRH) -  Snaclec rhodocytin subunit alpha from Calloselasma rhodostoma
Seq:
Struc:
136 a.a.
132 a.a.
Protein chains
Pfam   ArchSchema ?
Q9I840  (SLYB_CALRH) -  Snaclec rhodocytin subunit beta from Calloselasma rhodostoma
Seq:
Struc:
146 a.a.
122 a.a.
Key:    PfamA domain  Secondary structure  CATH domain

 

 
Biochemistry 47:7831-7837 (2008)
PubMed id: 18597489  
 
 
The crystal structure of the platelet activator aggretin reveals a novel (alphabeta)2 dimeric structure.
E.Hooley, E.Papagrigoriou, A.Navdaev, A.V.Pandey, J.M.Clemetson, K.J.Clemetson, J.Emsley.
 
  ABSTRACT  
 
Aggretin is a C-type lectin purified from Calloselasma rhodostoma snake venom. It is a potent activator of platelets, resulting in a collagen-like response by binding and clustering platelet receptor CLEC-2. We present here the crystal structure of aggretin at 1.7 A which reveals a unique tetrameric quaternary structure. The two alphabeta heterodimers are arranged through 2-fold rotational symmetry, resulting in an antiparallel side-by-side arrangement. Aggretin thus presents two ligand binding sites on one surface and can therefore cluster ligands in a manner reminiscent of convulxin and flavocetin. To examine the molecular basis of the interaction with CLEC-2, we used a molecular modeling approach of docking the aggretin alphabeta structure with the CLEC-2 N-terminal domain (CLEC-2N). This model positions the CLEC-2N structure face down in the "saddle"-shaped binding site which lies between the aggretin alpha and beta lectin-like domains. A 2-fold rotation of this complex to generate the aggretin tetramer reveals dimer contacts for CLEC-2N which bring the N- and C-termini into the proximity of each other, and a series of contacts involving two interlocking beta-strands close to the N-terminus are described. A comparison with homologous lectin-like domains from the immunoreceptor family reveals a similar but not identical dimerization mode, suggesting this structure may represent the clustered form of CLEC-2 capable of signaling across the platelet membrane.
 

Literature references that cite this PDB file's key reference

  PubMed id Reference
21098033 S.Séverin, A.Y.Pollitt, L.Navarro-Nuñez, C.A.Nash, D.Mourão-Sá, J.A.Eble, Y.A.Senis, and S.P.Watson (2011).
Syk-dependent phosphorylation of CLEC-2: a novel mechanism of hem-immunoreceptor tyrosine-based activation motif signaling.
  J Biol Chem, 286, 4107-4116.  
21277886 T.Sajevic, A.Leonardi, and I.Križaj (2011).
Haemostatically active proteins in snake venoms.
  Toxicon, 57, 627-645.  
20154214 A.Y.Pollitt, B.Grygielska, B.Leblond, L.Désiré, J.A.Eble, and S.P.Watson (2010).
Phosphorylation of CLEC-2 is dependent on lipid rafts, actin polymerization, secondary mediators, and Rac.
  Blood, 115, 2938-2946.  
19025564 C.Huysamen, and G.D.Brown (2009).
The fungal pattern recognition receptor, Dectin-1, and the associated cluster of C-type lectin-like receptors.
  FEMS Microbiol Lett, 290, 121-128.  
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.

 

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