The High Resolution NMR Structure of Parvulustat (Z‐2685) from Streptomyces parvulus FH‐1641: Comparison with Tendamistat from Streptomyces tendae 4158 |
| |
| Authors: | Stephan Rehm Sigeng Han Ismail Hassani Alma Sokocevic Hendrik R A Jonker Dr Joachim W Engels Prof Dr Harald Schwalbe Prof Dr |
| |
| Affiliation: | 1. Institute of Organic Chemistry and Chemical Biology, Center for Biomolecular Magnetic Resonance, Johann‐Wolfgang‐Goethe University, Max‐von‐Laue‐Strasse 7, 60438 Frankfurt am Main (Germany), Fax: (+49)?69‐79829515;2. Institute of Organic Chemistry and Chemical Biology, Johann‐Wolfgang‐Goethe University, Max‐von‐Laue‐Strasse 7, 60438 Frankfurt am Main (Germany) |
| |
| Abstract: | The protein parvulustat (Z‐2685) from Streptomyces parvulus comprises 78 amino acids and functions as a highly efficient α‐amylase inhibitor. Parvulustat shares 29.6 % overall amino acid sequence identity to the well‐known α‐amylase inhibitor tendamistat. Among the conserved residues are the two disulfide bridges (C9–C25, C43–C70) and the active‐site motif (W16, R17, Y18). Here, we report the high‐resolution NMR structure of parvulustat based on NOEs, J couplings, chemical shifts and hydrogen‐exchange data. In addition, we studied the dynamical properties of parvulustat by heteronuclear relaxation measurements. We compare the structure of parvulustat with the structure of tendamistat in terms of secondary structure elements, charges and hydrophobicity. The overall structural composition is very similar, but there are distinct differences including the active‐site region. These structural and dynamical differences indicate that for parvulustat an induced‐fit mechanism for binding to α‐amylase might take place, since the structure of tendamistat does not change upon binding to α‐amylase. |
| |
| Keywords: | inhibitors NMR spectroscopy parvulustat protein structure tendamistat |
|
|
