Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
1931577 | Biochemical and Biophysical Research Communications | 2010 | 5 Pages |
Angiotensin-I converting enzyme (ACE, a zinc dependent dipeptidyl carboxypeptidase) is a major target of drugs due to its role in the modulation of blood pressure and cardiovascular disorders. Here we present a crystal structure of AnCE (an ACE homologue from Drosophila melanogaster with a single enzymatic domain) in complex with a natural product-phosphonotripeptide, K-26 at 1.96 Å resolution. The inhibitor binds exclusively in the S1 and S2 binding pockets of AnCE (coordinating the zinc ion) through ionic and hydrogen bond interactions. A detailed structural comparison of AnCE·K-26 complex with individual domains of human somatic ACE provides useful information for further exploration of ACE inhibitor pharmacophores involving phosphonic acids.
Research highlights► This is first structure of AnCE (an ACE homologue) in complex with a natural peptide inhibitor K-26 ► K-26 binds exclusively at the non-prime binding pockets in the active site of AnCE ► High resolution crystal structure of AnCE·K-26 complex