標題: | Crystal Structure and Inhibition Studies of Transglutaminase from Streptomyces mobaraense |
作者: | Yang, Ming-Te Chang, Cheng-Hsiang Wang, Jiou Ming Wu, Tung Kung Wang, Yu-Kuo Chang, Chin-Yuan Li, TienHsiung Thomas 生物科技學系 Department of Biological Science and Technology |
公開日期: | 4-三月-2011 |
摘要: | The crystal structure of the microbial transglutaminase (MTGase) zymogen from Streptomyces mobaraense has been determined at 1.9-angstrom resolution using the molecular replacement method based on the crystal structure of the mature MTGase. The overall structure of this zymogen is similar to that of the mature form, consisting of a single disk-like domain with a deep active cleft at the edge of the molecule. A major portion of the prosequence (45 additional amino acid residues at the N terminus of the mature transglutaminase) folds into an L-shaped structure, consisting of an extended N-terminal segment linked with a one-turn short helix and a long alpha-helix. Two key residues in the short helix of the prosequence, Tyr-12 and Tyr-16, are located on top of the catalytic triad (Cys-110, Asp-301, and His-320) to block access of the substrate acyl donors and acceptors. Biochemical characterization of the mature MTGase, using N-alpha-benzyloxycarbonyl-L-glutaminylglycine as a substrate, revealed apparent K(m) and k(cat)/K(m) values of 52.66 mM and 40.42 mM(-1) min(-1), respectively. Inhibition studies using the partial prosequence SYAETYR and homologous sequence SQAETYR showed a noncompetitive inhibition mechanism with IC(50) values of 0.75 and 0.65 mM, respectively, but no cross-linking product formation. Nevertheless, the prosequence homologous oligopeptide SQAETQR, with Tyr-12 and Tyr-16 each replaced with Gln, exhibited inhibitory activity with the formation of the SQAETQR-monodansylcadaverine fluorophore cross-linking product (SQAETQR-C-DNS). MALDI-TOF tandem MS analysis of SQAETQR-C-DNS revealed molecular masses corresponding to those of (N)SQAETQ(C)-C-DNS and C-DNS-(N)QR(C) sequences, suggesting the incorporation of C-DNS onto the C-terminal Gln residue of the prosequence homologous oligopeptide. These results support the putative functional roles of both Tyr residues in substrate binding and inhibition. |
URI: | http://dx.doi.org/10.1074/jbc.M110.203315 http://hdl.handle.net/11536/9156 |
ISSN: | 0021-9258 |
DOI: | 10.1074/jbc.M110.203315 |
期刊: | JOURNAL OF BIOLOGICAL CHEMISTRY |
Volume: | 286 |
Issue: | 9 |
起始頁: | 7301 |
結束頁: | 7307 |
顯示於類別: | 期刊論文 |