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Literature DB >> 17079133

Docking interactions in protein kinase and phosphatase networks.

Attila Reményi¹, Matthew C Good, Wendell A Lim.

Abstract

To achieve high biological specificity, protein kinases and phosphatases often recognize their targets through interactions that occur outside of the active site. Although the role of modular protein-protein interaction domains in kinase and phosphatase signaling has been well characterized, it is becoming clear that many kinases and phosphatases utilize docking interactions - recognition of a short peptide motif in target partners by a groove on the catalytic domain that is separate from the active site. Docking is particularly prevalent in serine/threonine kinases and phosphatases, and is a versatile organizational tool for building complex signaling networks; it confers a high degree of specificity and, in some cases, allosteric regulation.

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Year: 2006 PMID： 17079133 DOI： 10.1016/j.sbi.2006.10.008

Source DB: PubMed Journal: Curr Opin Struct Biol ISSN： 0959-440X Impact factor: 6.809

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Cited

86 in total

1. Examining docking interactions on ERK2 with modular peptide substrates.

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Journal: Biochemistry Date: 2011-10-18 Impact factor: 3.162

2. Two hydrophobic residues can determine the specificity of mitogen-activated protein kinase docking interactions.

Authors: A Jane Bardwell; Lee Bardwell
Journal: J Biol Chem Date: 2015-09-14 Impact factor: 5.157

Review 3. Understanding and exploiting substrate recognition by protein kinases.

Authors: Benjamin E Turk
Journal: Curr Opin Chem Biol Date: 2008-03-07 Impact factor: 8.822

4. Selectivity of docking sites in MAPK kinases.

Authors: A Jane Bardwell; Erlynn Frankson; Lee Bardwell
Journal: J Biol Chem Date: 2009-02-05 Impact factor: 5.157

5. Distal recognition sites in substrates are required for efficient phosphorylation by the cAMP-dependent protein kinase.

Authors: Stephen J Deminoff; Vidhya Ramachandran; Paul K Herman
Journal: Genetics Date: 2009-04-13 Impact factor: 4.562

Docking interactions in protein kinase and phosphatase networks.

1. Examining docking interactions on ERK2 with modular peptide substrates.

2. Two hydrophobic residues can determine the specificity of mitogen-activated protein kinase docking interactions.

Review 3. Understanding and exploiting substrate recognition by protein kinases.

4. Selectivity of docking sites in MAPK kinases.

5. Distal recognition sites in substrates are required for efficient phosphorylation by the cAMP-dependent protein kinase.

6. Threonine phosphorylation prevents promoter DNA binding of the Group B Streptococcus response regulator CovR.

7. Chemoproteomic Profiling Uncovers CDK4-Mediated Phosphorylation of the Translational Suppressor 4E-BP1.

8. Conformational snapshots of Tec kinases during signaling.

9. Structure and substrate recruitment of the human spindle checkpoint kinase Bub1.

10. Itk tyrosine kinase substrate docking is mediated by a nonclassical SH2 domain surface of PLCgamma1.