Catalytic domain crystal structure of protein kinase C-θ (PKC θ)

被引:126
|
作者
Xu, ZB
Chaudhary, D
Olland, S
Wolfrom, S
Czerwinski, R
Malakian, K
Lin, L
Stahl, ML
McCarthy, DJ
Benander, C
Fitz, L
Greco, R
Somers, WS
Mosyak, L
机构
[1] Wyeth Ayerst Res, Dept Chem & Screening Sci, Cambridge, MA 02140 USA
[2] Wyeth Ayerst Res, Inflammat Dept, Cambridge, MA 02140 USA
关键词
D O I
10.1074/jbc.M409216200
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
A member of the novel protein kinase C (PKC) subfamily, PKCtheta, is an essential component of the T cell synapse and is required for optimal T cell activation and interleukin-2 production. Selective involvement of PKCtheta in TCR signaling makes this enzyme an attractive therapeutic target in T cell-mediated disease processes. In this report we describe the crystal structure of the catalytic domain of PKCtheta at 2.0-resolution. Human recombinant PKCtheta kinase domain was expressed in bacteria as catalytically active phosphorylated enzyme and co-crystallized with its subnanomolar, ATP site inhibitor staurosporine. The structure follows the classic bilobal kinase fold and shows the enzyme in its active conformation and phosphorylated state. Inhibitory interactions between conserved features of staurosporine and the ATP-binding cleft are accompanied by closing of the glycine-rich loop, which also maintains an inhibitory arrangement by blocking the phosphate recognition sub-site. The two major phosphorylation sites, Thr-538 in the activation loop and Ser-695 in the hydrophobic motif, are both occupied in the structure, playing key roles in stabilizing active conformation of the enzyme and indicative of PKCtheta autocatalytic phosphorylation and activation during bacterial expression. The PKCtheta-staurosporine complex represents the first kinase domain crystal structure of any PKC isotypes to be determined and as such should provide valuable insight into PKC specificity and into rational drug design strategies for PKCtheta selective leads.
引用
收藏
页码:50401 / 50409
页数:9
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