PDBsum entry 1bmm

Hydrolase/hydrolase inhibitor

PDB id: 1bmm

Contents

Protein chains

28 a.a. *

258 a.a. *

Ligands

ASP-PHE-GLU-GLU-ILE-PRO-GLU-GLU-TYR

BM2

Waters ×42

* Residue conservation analysis

PDB id:

1bmm

Name:

Hydrolase/hydrolase inhibitor

Title:

Human alpha-thrombin complexed with [s-(r ,R )]-4-[(Aminoiminomethyl) amino]-n-[[1-[3-hydroxy-2-[(2-naphthalenylsulfonyl)amino]-1- oxopropyl]-2-pyrrolidinyl] methyl]butanamide (bms-186282)

Structure:

Alpha-thrombin. Chain: l. Alpha-thrombin. Chain: h. Hirudin i. Chain: i

Source:

Homo sapiens. Human. Organism_taxid: 9606. Tissue: plasma. Hirudo medicinalis. Medicinal leech. Organism_taxid: 6421. Tissue: plasma

Biol. unit:

Trimer (from PQS)

Resolution:

2.60Å R-factor: 0.177

Authors:

M.Malley,J.Sack

Key ref:

M.F.Malley et al. (1996). Crystallographic determination of the structures of human alpha-thrombin complexed with BMS-186282 and BMS-189090. Protein Sci, 5, 221-228. PubMed id: 8745399 DOI: 10.1002/pro.5560050205

Date:

14-Nov-95 Release date: 07-Dec-96

Protein chain

P00734  (THRB_HUMAN) -  Prothrombin from Homo sapiens

Seq: 622 a.a.

Struc: 28 a.a.

Protein chain

P00734  (THRB_HUMAN) -  Prothrombin from Homo sapiens

Seq: 622 a.a.

Struc: 258 a.a.

Enzyme reactions

• Enzyme class: Chains L, H: E.C.3.4.21.5 - thrombin.
• Reaction: Preferential cleavage: Arg-|-Gly; activates fibrinogen to fibrin and releases fibrinopeptide A and B.

DOI no: 10.1002/pro.5560050205

Protein Sci 5:221-228 (1996)

PubMed id: 8745399

Crystallographic determination of the structures of human alpha-thrombin complexed with BMS-186282 and BMS-189090.

M.F.Malley, L.Tabernero, C.Y.Chang, S.L.Ohringer, D.G.Roberts, J.Das, J.S.Sack.

ABSTRACT

The crystallographic structures of the ternary complexes of human alpha-thrombin with hirugen (a sulfated hirudin fragment) and the small-molecule active site thrombin inhibitors BMS-186282 and BMS-189090 have been determined at 2.6 and 2.8 A. In both cases, the inhibitors, which adopt very similar bound conformations, bind in an antiparallel beta-strand arrangement relative to the thrombin main chain in a manner like that reported for PPACK, D-Phe-Pro-Arg-CH2Cl. They do, however, exhibit differences in the binding of the alkyl guanidine moiety in the specificity pocket. Numerous hydrophilic and hydrophobic interactions serve to stabilize the inhibitors in the binding pocket. Although PPACK forms covalent bonds to both serine and the histidine of the catalytic triad of thrombin, neither BMS-186282 nor BMS-189090 bind covalently and only BMS-186282 forms a hydrogen bond to the serine of the catalytic triad. Both inhibitors bind with high affinity (Ki = 79 nM and 3.6 nM, respectively) and are highly selective for thrombin over trypsin and other serine proteases.

Selected figure(s)

Figure 1.
Fig. 1. Structures of PPACK andNAPAPand the development of BMS-186282 and BMS-189090 from MD-805 and BMS-183507.

Figure 4.
Fig. 4. Final (2F, - F, I omitelectrondensitymaps at the active of cy-thrombincomplexedwith (A) BMS-186282 and (B) BMS-189D90 su- perimposewiththefinalthree-dimensionalstructures of the inhibitors. Electron densitymapswerecalculatedusingX-PLOR(Briinger,1989).

The above figures are reprinted from an Open Access publication published by the Protein Society: Protein Sci (1996, 5, 221-228) copyright 1996.