Phosphoprotein and phosphopeptide interactions with the FHA domain from arabidopsis kinase-associated protein phosphatase

被引:42
作者
Ding, Zhaofeng
Wang, Huachun
Liang, Xiangyang
Morris, Erin R.
Gallazzi, Fabio
Pandit, Shashi
Skolnick, Jeffrey
Walker, John C.
Van Doren, Steven R.
机构
[1] Univ Missouri, Dept Biochem, Div Biol Sci, Columbia, MO 65211 USA
[2] Univ Missouri, Bond Life Sci Ctr, Columbia, MO 65211 USA
关键词
D O I
10.1021/bi061763n
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
FHA domains are phospho Thr recognition modules found in diverse signaling proteins, including kinase-associated protein phosphatase ( KAPP) from Arabidopsis thaliana. The kinase-interacting FHA domain (KI-FHA) of KAPP targets it to function as a negative regulator of some receptor-like kinase (RLK) signaling pathways important in plant development and environmental responses. To aid in the identification of potential binding sites for the KI-FHA domain, we predicted (i) the structure of a representative KAPP-binding RLK, CLAVATA1, and (ii) the functional surfaces of RLK kinase domains using evolutionary trace analysis. We selected phosphopeptides from KAPP-binding Arabidopsis RLKs for in vitro studies of association with KI-FHA from KAPP. Three phospho Thr peptide fragments from the kinase domain of CLV1 or BAK1 were found to bind KI-FHA with K-D values of 8-20 mu M, by NMR or titration calorimetry. Their affinity is driven by favorable enthalpy and solvation entropy gain. Mutagenesis of these three threonine sites suggests Thr546 in the C-lobe of the BAK1 kinase domain to be a principal but not sole site of KI-FHA binding in vitro. The brassinosteroid receptor BRI1 and KAPP are shown to associate in vivo and in vitro. Further genetic studies indicate that KAPP may be a negative regulator of the BRI1 signaling transduction pathway. N-15-Labeled KI-FHA was titrated with the GSTBRI1 kinase domain and monitored by NMR. BRI1 interacts with the same 3/4, 4/5, 6/7, 8/9, and 10/11 recognition loops of KI-FHA, with similar affinity as the phospho Thr peptides.
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页码:2684 / 2696
页数:13
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