Molecular Mechanisms of Tight Binding through Fuzzy Interactions |
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| Authors: | Qingliang Shen Jie Shi Danyun Zeng Baoyu Zhao Pingwei Li Wonmuk Hwang Jae-Hyun Cho |
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| Affiliation: | 1. Department of Biochemistry and Biophysics, Texas A&M University, College Station, Texas;2. Department of Biomedical Engineering, Texas A&M University, College Station, Texas;3. Department of Materials Science and Engineering, Texas A&M University, College Station, Texas;4. School of Computational Sciences, Korea Institute for Advanced Study, Seoul, South Korea |
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| Abstract: | ![]()
Many intrinsically disordered proteins (IDPs) form fuzzy complexes upon binding to their targets. Although many IDPs are weakly bound in fuzzy complexes, some IDPs form high-affinity complexes. One example is the nonstructural protein 1 (NS1) of the 1918 Spanish influenza A virus, which hijacks cellular CRKII through the strong binding affinity (Kd ~10 nM) of its proline-rich motif (PRMNS1) to the N-terminal Src-homology 3 domain of CRKII. However, its molecular mechanism remains elusive. Here, we examine the interplay between structural disorder of a bound PRMNS1 and its long-range electrostatic interactions. Using x-ray crystallography and NMR spectroscopy, we found that PRMNS1 retains substantial conformational flexibility in the bound state. Moreover, molecular dynamics simulations showed that structural disorder of the bound PRMNS1 increases the number of electrostatic interactions and decreases the mean distances between the positively charged residues in PRMNS1 and the acidic residues in the N-terminal Src-homology 3 domain. These results are analyzed using a polyelectrostatic model. Our results provide an insight into the molecular recognition mechanism for a high-affinity fuzzy complex. |
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| Keywords: | Corresponding author |
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