?
2014.06.16,我院周叢照和陳宇星教授研究組和美國UAB的吳輝教授研究組合作在Journal of Biological Chemistry上在線發(fā)表論文:Structure of a novel O-GlcNAc transferase GtfA reveals insights into the glycosylation of pneumococcal serine-rich repeat adhesins. 2014 Jun 16. pii: jbc.M114.581934.
作者:師偉偉#��、江永亮#、Zhu Fan���、楊益虎����、邵秋燕�����、楊海濱���、任艷敏、吳輝*��、陳宇星*�����、周叢照*�。
Abstract:Protein glycosylation catalyzed by the O-GlcNAc transferase (OGT) plays a critical role in various biological processes. In Streptococcus pneumoniae, the core enzyme GtfA and co-activator GtfB form an OGT complex to glycosylate the serine-rich repeat (SRR) of adhesin PsrP, which is involved in the infection and pathogenesis. Here we report the 2.0-? crystal structure of GtfA, revealing a β-meander add-on domain beyond the catalytic domain. It represents a novel add-on domain, which is distinct from the all-α tetratricopeptide repeats in the only two structure-known OGTs. Structural analyses combined with binding assays indicate that this add-on domain contributes to forming an active GtfA-GtfB complex and recognizing the acceptor protein. In addition, the in vitro glycosylation system enables us to map the O-linkages to the serine residues within the first SRR of PsrP. These findings suggest that fusion with an add-on domain might be a universal mechanism for diverse OGTs that recognize varying acceptor proteins/peptides.
版權(quán)與免責(zé)聲明:本網(wǎng)頁的內(nèi)容由收集互聯(lián)網(wǎng)上公開發(fā)布的信息整理獲得。目的在于傳遞信息及分享����,并不意味著贊同其觀點(diǎn)或證實(shí)其真實(shí)性���,也不構(gòu)成其他建議。僅提供交流平臺(tái)�,不為其版權(quán)負(fù)責(zé)。如涉及侵權(quán)���,請聯(lián)系我們及時(shí)修改或刪除�。郵箱:sales@allpeptide.com