| Literature DB >> 25131700 |
Qiong Xing1, Peng Huang, Ju Yang, Jian-Qiang Sun, Zhou Gong, Xu Dong, Da-Chuan Guo, Shao-Min Chen, Yu-Hong Yang, Yan Wang, Ming-Hui Yang, Ming Yi, Yi-Ming Ding, Mai-Li Liu, Wei-Ping Zhang, Chun Tang.
Abstract
Proteins interact with each other to fulfill their functions. The importance of weak protein-protein interactions has been increasingly recognized. However, owing to technical difficulties, ultra-weak interactions remain to be characterized. Phosphorylation can take place via a K(D)≈25 mM interaction between two bacterial enzymes. Using paramagnetic NMR spectroscopy and with the introduction of a novel Gd(III)-based probe, we determined the structure of the resulting complex to atomic resolution. The structure accounts for the mechanism of phosphoryl transfer between the two enzymes and demonstrates the physical basis for their ultra-weak interaction. Further, molecular dynamics (MD) simulations suggest that the complex has a lifetime in the micro- to millisecond regimen. Hence such interaction is termed a fleeting interaction. From mathematical modeling, we propose that an ultra-weak fleeting interaction enables rapid flux of phosphoryl signal, providing a high effective protein concentration.Keywords: NMR spectroscopy; paramagnetic relaxation enhancement; protein-protein interactions; proteins; signal transduction
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Year: 2014 PMID: 25131700 DOI: 10.1002/anie.201405976
Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN: 1433-7851 Impact factor: 15.336