1VSB
SUBTILISIN CARLSBERG L-PARA-CHLOROPHENYL-1-ACETAMIDO BORONIC ACID INHIBITOR COMPLEX
Summary for 1VSB
| Entry DOI | 10.2210/pdb1vsb/pdb |
| Descriptor | SUBTILISIN CARLSBERG, TYPE VIII (2 entities in total) |
| Functional Keywords | serine protease, hydrolase, boronic acid inhibitors |
| Biological source | Bacillus licheniformis |
| Cellular location | Secreted: P00780 |
| Total number of polymer chains | 1 |
| Total formula weight | 27546.67 |
| Authors | Stoll, V.S.,Eger, B.T.,Hynes, R.C.,Martichonok, V.,Jones, J.B.,Pai, E.F. (deposition date: 1997-09-17, release date: 1998-03-18, Last modification date: 2023-08-09) |
| Primary citation | Stoll, V.S.,Eger, B.T.,Hynes, R.C.,Martichonok, V.,Jones, J.B.,Pai, E.F. Differences in binding modes of enantiomers of 1-acetamido boronic acid based protease inhibitors: crystal structures of gamma-chymotrypsin and subtilisin Carlsberg complexes. Biochemistry, 37:451-462, 1998 Cited by PubMed Abstract: In order to probe the structural basis of stereoselectivity in the serine protease family, a series of enantiomeric boronic acids RCH2CH(NHCOCH3)B(OH)2 has been synthesized and kinetically characterized as transition-state analog inhibitors using alpha-chymotrypsin and subtilisin Carlsberg as model systems. When the R-substituent in this series was changed from a p-chlorophenyl to a 1-naphthyl group, alpha-chymotrypsin, but not subtilisin, reversed its usual preference for l-enantiomers and bound more tightly to the D-enantiomer [Martichonok, V., & Jones, J. B. (1996) J. Am. Chem. Soc. 118, 950-958]. The structural factors responsible for the differences in stereoselectivity between the two enzymes have been explored by X-ray crystallographic examination of subtilisin Carlsberg and gamma-chymotrypsin complexes of the L- and D-enantiomers of p-chlorophenyl and 1-naphthyl boronic acid derivatives. In both enzymes, the L-isomers of the inhibitors, which are more closely related to the natural L-amino acid substrates, form tetrahedral adducts, covalently linking the central boron atom and Ogamma of the catalytic serine. The d-isomers, however, differ in the way they interact with subtilisin or gamma-chymotrypsin. With subtilisin, both the D-p-chlorophenyl and D-1-naphthyl inhibitor complexes form covalent Ser Ogamma-to-boron bonds, but with gamma-chymotrypsin, the same inhibitors lead to novel tetrahedral adducts covalently linking both Ser195 Ogamma and His57 Nepsilon2 covalently via the boron atom. PubMed: 9425066DOI: 10.1021/bi971166o PDB entries with the same primary citation |
| Experimental method | X-RAY DIFFRACTION (2.1 Å) |
Structure validation
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