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PDBsum entry 4zxy
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protein ligands metals Protein-protein interface(s) links
Hydrolase/hydrolase inhibitor PDB id
4zxy

 

 

 

 

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Contents
Protein chains
250 a.a.
55 a.a.
Ligands
4T1
SO4 ×3
GOL
Metals
_CA
Waters ×196
PDB id:
4zxy
Name: Hydrolase/hydrolase inhibitor
Title: Factor viia in complex with the inhibitor (2r)-2-[(1-aminoisoquinolin- 6-yl)amino]-4,11-diazatricyclo[14.2.2.1~6,10~]henicosa-1(18),6(21),7, 9,16,19-hexaene-3,12-dione
Structure: Coagulation factor viia heavy chain. Chain: h. Fragment: unp residues 213-466. Synonym: proconvertin,serum prothrombin conversion accelerator,spca. Engineered: yes. Coagulation factor viia light chain. Chain: l. Fragment: unp residues 150-204. Synonym: proconvertin,serum prothrombin conversion accelerator,spca.
Source: Homo sapiens. Human. Organism_taxid: 9606. Gene: f7. Expressed in: cricetinae. Expression_system_taxid: 10026. Expression_system_taxid: 10026
Resolution:
2.06Å     R-factor:   0.192     R-free:   0.211
Authors: A.Wei
Key ref: E.S.Priestley et al. (2015). Structure-Based Design of Macrocyclic Coagulation Factor VIIa Inhibitors. J Med Chem, 58, 6225-6236. PubMed id: 26151189 DOI: 10.1021/acs.jmedchem.5b00788
Date:
20-May-15     Release date:   22-Jul-15    
PROCHECK
Go to PROCHECK summary
 Headers
 References

Protein chain
Pfam   ArchSchema ?
P08709  (FA7_HUMAN) -  Coagulation factor VII from Homo sapiens
Seq:
Struc: 		466 a.a.
250 a.a.
Protein chain
Pfam   ArchSchema ?
P08709  (FA7_HUMAN) -  Coagulation factor VII from Homo sapiens
Seq:
Struc: 		466 a.a.
55 a.a.
Key:    PfamA domain  Secondary structure  CATH domain

 Enzyme reactions 
   Enzyme class: Chains H, L: E.C.3.4.21.21  - coagulation factor VIIa.
[IntEnz]   [ExPASy]   [KEGG]   [BRENDA]
      Reaction: Hydrolyzes one Arg-|-Ile bond in factor X to form factor Xa.

 

 
DOI no: 10.1021/acs.jmedchem.5b00788 J Med Chem 58:6225-6236 (2015)
PubMed id: 26151189  
 
 
Structure-Based Design of Macrocyclic Coagulation Factor VIIa Inhibitors.
E.S.Priestley, D.L.Cheney, I.DeLucca, A.Wei, J.M.Luettgen, A.R.Rendina, P.C.Wong, R.R.Wexler.
 
  ABSTRACT  
 
On the basis of a crystal structure of a phenylpyrrolidine lead and subsequent molecular modeling results, we designed and synthesized a novel series of macrocyclic FVIIa inhibitors. The optimal 16-membered macrocycle was 60-fold more potent than an acyclic analog. Further potency optimization by incorporation of P1' alkyl sulfone and P2 methyl groups provided a macrocycle with TF/FVIIa Ki = 1.6 nM, excellent selectivity against a panel of seven serine proteases, and FVII-deficient prothrombin time EC2x = 1.2 μM. Discovery of this potent, selective macrocyclic scaffold opens new possibilities for the development of orally bioavailable FVIIa inhibitors.
 

 

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