Structural studies of PI3K SH3 domain in complex with a peptide ligand: role of anchor residue in ligand binding

Batra-Safferling, R.; Granzin, J.; Moedder, S.; Hoffmann, S.; Willbold, D.

doi:10.1515/bc.2010.003

Journal Article

Structural studies of PI3K SH3 domain in complex with a peptide ligand: role of anchor residue in ligand binding

Batra-Safferling, R.FZJ* ; Granzin, J.FZJ* ; Moedder, S.FZJ* ; Hoffmann, S.FZJ* ; Willbold, D.FZJ*

2010
de Gruyter Berlin [u.a.]

Biological chemistry 391, 33 - 42 (2010) [10.1515/bc.2010.003]

This record in other databases:

Please use a persistent id in citations: http://hdl.handle.net/2128/18353 doi:10.1515/BC.2010.003

Abstract: Src homology 3 (SH3) domains are mediators of protein-protein interactions. They comprise approximately 60 amino acid residues and are found in many intracellular signaling proteins. Here, we present the crystal structure of the SH3 domain from phosphatidylinositol 3-kinase (PI3K) in complex with the 12-residue proline-rich peptide PD1R (HSKRPLPPLPSL). The crystal structure of the PI3K SH3-PD1R complex at a resolution of 1.7 A reveals type I ligand orientation of the bound peptide with an extended conformation where the central portion forms a left-handed type II polyproline (PPII) helix. The overall structure of the SH3 domain shows minimal changes on ligand binding. In addition, we also attempted crystallization with another peptide ligand (PD1) where the residue at anchor position P(-3) is a tyrosine. The crystals obtained did not contain the PD1 ligand; instead, the ligand binding site is partially occupied by residues Arg18 and Trp55 from the symmetry-related PI3K SH3 molecule. Considering these crystal structures of PI3K SH3 together with published reports, we provide a comparative analysis of protein-ligand interactions that has helped us identify the individual residues which play an important role in defining target specificity.

Keyword(s): Amino Acid Sequence (MeSH) ; Binding Sites (MeSH) ; Crystallography, X-Ray (MeSH) ; Ligands (MeSH) ; Models, Molecular (MeSH) ; Molecular Sequence Data (MeSH) ; Oligopeptides: metabolism (MeSH) ; Peptides: chemistry (MeSH) ; Phosphatidylinositol 3-Kinases: chemistry (MeSH) ; Phosphatidylinositol 3-Kinases: metabolism (MeSH) ; Protein Binding (MeSH) ; src Homology Domains: physiology (MeSH) ; Ligands ; Oligopeptides ; Peptides ; histidyl-seryl-lysyl-arginyl-prolyl-leucyl-prolyl-prolyl-leucyl-prolyl-seryl-leucine ; polyproline ; Phosphatidylinositol 3-Kinases ; J ; phosphatidylinositol 3-kinase (auto) ; polyproline helix (auto) ; protein-ligand interaction (auto) ; Src homology 3 (auto) ; pi stacking (auto)

Classification:

Biochemistry & Molecular Biology

Note: The authors wish to thank Georg Buldt for continuous generous support. Furthermore, technical assistance by Esther Jonas and the beamline scientists at the ESRF (Grenoble, France) is acknowledged. We also thank Oliver Weiergraber for critical reading of the manuscript. This work was supported by a grant from the Deutsche Forschungsgemeinschaft (SFB 575, B11) to D.W.

Contributing Institute(s):

Research Program(s):

Appears in the scientific report 2010

Database coverage:
OpenAccess

Click to display QR Code for this record

The record appears in these collections:
Document types > Articles > Journal Article
JARA > JARA > JARA-JARA\-HPC
Institute Collections > IBI > IBI-7
Workflow collections > Public records
ICS > ICS-6
Publications database
Open Access

Record created 2012-11-13, last modified 2020-04-23

Similar records

OpenAccess:

PDF
External link:

Fulltext by OpenAccess repository

Rate this document:

(Not yet reviewed)

Add to personal basket
Export as Author List with IDs BibTeX (UTF-8), EndNote XML, EndNote Text, RIS, MARC, Print MARC, MARCXML, DC,
Request correction
Submit fulltext

guest :: login JuSER
		Search		Submit		Personalize Your alerts Your baskets Your searches		Help