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Literature DB >> 20442417

Loops govern SH2 domain specificity by controlling access to binding pockets.

Tomonori Kaneko¹, Haiming Huang, Bing Zhao, Lei Li, Huadong Liu, Courtney K Voss, Chenggang Wu, Martin R Schiller, Shawn Shun-Cheng Li.

Abstract

Cellular functions require specific protein-protein interactions that are often mediated by modular domains that use binding pockets to engage particular sequence motifs in their partners. Yet, how different members of a domain family select for distinct sequence motifs is not fully understood. The human genome encodes 120 Src homology 2 (SH2) domains (in 110 proteins), which mediate protein-protein interactions by binding to proteins with diverse phosphotyrosine (pTyr)-containing sequences. The structure of the SH2 domain of BRDG1 bound to a peptide revealed a binding pocket that was blocked by a loop residue in most other SH2 domains. Analysis of 63 SH2 domain structures suggested that the SH2 domains contain three binding pockets, which exhibit selectivity for the three positions after the pTyr in a peptide, and that SH2 domain loops defined the accessibility and shape of these pockets. Despite sequence variability in the loops, we identified conserved structural features in the loops of SH2 domains responsible for controlling access to these surface pockets. We engineered new loops in an SH2 domain that altered specificity as predicted. Thus, selective blockage of binding subsites or pockets by surface loops provides a molecular basis by which the diverse modes of ligand recognition by the SH2 domain may have evolved and provides a framework for engineering SH2 domains and designing SH2-specific inhibitors.

Entities: CellLine Chemical Disease Gene Mutation Species

Mesh：

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Year: 2010 PMID： 20442417 PMCID： PMC6590088 DOI： 10.1126/scisignal.2000796

Source DB: PubMed Journal: Sci Signal ISSN： 1945-0877 Impact factor: 8.192

85 in total

1. STRAP: editor for STRuctural Alignments of Proteins.

Authors: C Gille; C Frömmel
Journal: Bioinformatics Date: 2001-04 Impact factor: 6.937

2. Structural basis for specificity switching of the Src SH2 domain.

Authors: M S Kimber; J Nachman; A M Cunningham; G D Gish; T Pawson; E F Pai
Journal: Mol Cell Date: 2000-06 Impact factor: 17.970

3. The top loops of the C(2) domains from synaptotagmin and phospholipase A(2) control functional specificity.

Authors: S H Gerber; J Rizo; T C Südhof
Journal: J Biol Chem Date: 2001-07-10 Impact factor: 5.157

4. Crystal structures of the XLP protein SAP reveal a class of SH2 domains with extended, phosphotyrosine-independent sequence recognition.

Authors: F Poy; M B Yaffe; J Sayos; K Saxena; M Morra; J Sumegi; L C Cantley; C Terhorst; M J Eck
Journal: Mol Cell Date: 1999-10 Impact factor: 17.970

5. Solution structure of the SH2 domain of Grb2 complexed with the Shc-derived phosphotyrosine-containing peptide.

Authors: K Ogura; S Tsuchiya; H Terasawa; S Yuzawa; H Hatanaka; V Mandiyan; J Schlessinger; F Inagaki
Journal: J Mol Biol Date: 1999-06-11 Impact factor: 5.469

6. Molecular cloning of murine STAP-1, the stem-cell-specific adaptor protein containing PH and SH2 domains.

Authors: M Masuhara; K Nagao; M Nishikawa; M Sasaki; A Yoshimura; M Osawa
Journal: Biochem Biophys Res Commun Date: 2000-02-24 Impact factor: 3.575

7. Structure of the amino-terminal domain of Cbl complexed to its binding site on ZAP-70 kinase.

Authors: W Meng; S Sawasdikosol; S J Burakoff; M J Eck
Journal: Nature Date: 1999-03-04 Impact factor: 49.962

8. Novel mode of ligand binding by the SH2 domain of the human XLP disease gene product SAP/SH2D1A.

Authors: S C Li; G Gish; D Yang; A J Coffey; J D Forman-Kay; I Ernberg; L E Kay; T Pawson
Journal: Curr Biol Date: 1999-12-02 Impact factor: 10.834

9. Molecular cloning of a docking protein, BRDG1, that acts downstream of the Tec tyrosine kinase.

Authors: K Ohya; S Kajigaya; A Kitanaka; K Yoshida; A Miyazato; Y Yamashita; T Yamanaka; U Ikeda; K Shimada; K Ozawa; H Mano
Journal: Proc Natl Acad Sci U S A Date: 1999-10-12 Impact factor: 11.205

10. A motif-based profile scanning approach for genome-wide prediction of signaling pathways.

Authors: M B Yaffe; G G Leparc; J Lai; T Obata; S Volinia; L C Cantley
Journal: Nat Biotechnol Date: 2001-04 Impact factor: 54.908

39 in total

1. Mechanism of phosphorylation-induced activation of phospholipase C-gamma isozymes.

Authors: Aurelie Gresset; Stephanie N Hicks; T Kendall Harden; John Sondek
Journal: J Biol Chem Date: 2010-08-31 Impact factor: 5.157

2. Crucial roles of single residues in binding affinity, specificity, and promiscuity in the cellulosomal cohesin-dockerin interface.

Authors: Michal Slutzki; Dan Reshef; Yoav Barak; Rachel Haimovitz; Shahar Rotem-Bamberger; Raphael Lamed; Edward A Bayer; Ora Schueler-Furman
Journal: J Biol Chem Date: 2015-04-01 Impact factor: 5.157

Review 3. Designing specific protein-protein interactions using computation, experimental library screening, or integrated methods.

Authors: T Scott Chen; Amy E Keating
Journal: Protein Sci Date: 2012-06-08 Impact factor: 6.725

Loops govern SH2 domain specificity by controlling access to binding pockets.

1. STRAP: editor for STRuctural Alignments of Proteins.

2. Structural basis for specificity switching of the Src SH2 domain.

3. The top loops of the C(2) domains from synaptotagmin and phospholipase A(2) control functional specificity.

4. Crystal structures of the XLP protein SAP reveal a class of SH2 domains with extended, phosphotyrosine-independent sequence recognition.

5. Solution structure of the SH2 domain of Grb2 complexed with the Shc-derived phosphotyrosine-containing peptide.

6. Molecular cloning of murine STAP-1, the stem-cell-specific adaptor protein containing PH and SH2 domains.

7. Structure of the amino-terminal domain of Cbl complexed to its binding site on ZAP-70 kinase.

8. Novel mode of ligand binding by the SH2 domain of the human XLP disease gene product SAP/SH2D1A.

9. Molecular cloning of a docking protein, BRDG1, that acts downstream of the Tec tyrosine kinase.

10. A motif-based profile scanning approach for genome-wide prediction of signaling pathways.

1. Mechanism of phosphorylation-induced activation of phospholipase C-gamma isozymes.

2. Crucial roles of single residues in binding affinity, specificity, and promiscuity in the cellulosomal cohesin-dockerin interface.

Review 3. Designing specific protein-protein interactions using computation, experimental library screening, or integrated methods.

4. Surface Loops in a Single SH2 Domain Are Capable of Encoding the Spectrum of Specificity of the SH2 Family.

5. Engineered SH2 domains with tailored specificities and enhanced affinities for phosphoproteome analysis.

6. Tyrosine phosphorylation of the Lyn Src homology 2 (SH2) domain modulates its binding affinity and specificity.

7. Structural insights into the intertwined dimer of fyn SH2.

8. Dynamically Coupled Residues within the SH2 Domain of FYN Are Key to Unlocking Its Activity.

Review 9. Evolution of SH2 domains and phosphotyrosine signalling networks.

10. Specificity of linear motifs that bind to a common mitogen-activated protein kinase docking groove.