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Published online before print December 22, 2006, 10.1110/ps.062496807
Protein Science (2007), 16:189-196. Published by Cold Spring Harbor Laboratory Press. Copyright © 2007 The Protein Society
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The SH3 domain of a M7 interacts with its C-terminal proline-rich region

Qinghua Wang1,4, Matthew A. Deloia2,4, Yang Kang1,3, Casey Litchke1, Naixia Zhang1, Margaret A. Titus2, and Kylie J. Walters1

1 Department of Biochemistry, Molecular Biology and Biophysics, University of Minnesota, Minneapolis, Minnesota 55455, USA
2 Department of Genetics, Cell Biology, and Development, University of Minnesota, Minneapolis, Minnesota 55455, USA
3 Department of Oral Sciences, University of Minnesota, Minneapolis, Minnesota 55455, USA

(RECEIVED August 14, 2006; FINAL REVISION October 27, 2006; ACCEPTED October 28, 2006)

Myosins play essential roles in migration, cytokinesis, endocytosis, and adhesion. They are composed of a large N-terminal motor domain with ATPase and actin binding sites and C-terminal neck and tail regions, whose functional roles and structural context in the protein are less well characterized. The tail regions of myosins I, IV, VII, XII, and XV each contain a putative SH3 domain that may be involved in protein–protein interactions. SH3 domains are reported to bind proline-rich motifs, especially "PxxP" sequences, and such interactions serve regulatory functions. The activity of Src, PI3, and Itk kinases, for example, is regulated by intramolecular interactions between their SH3 domain and internal proline-rich sequences. Here, we use NMR spectroscopy to reveal the structure of a protein construct from Dictyostelium myosin VII (DdM7) spanning A1620–T1706, which contains its SH3 domain and adjacent proline-rich region. The SH3 domain forms the signature beta-barrel architecture found in other SH3 domains, with conserved tryptophan and tyrosine residues forming a hydrophobic pocket known to bind "PxxP" motifs. In addition, acidic residues in the RT or n–Src loops are available to interact with the basic anchoring residues that are typically found in ligands or proteins that bind SH3 domains. The DdM7 SH3 differs in the hydrophobicity of the second pocket formed by the 310 helix and following beta-strand, which contains polar rather than hydrophobic side chains. Most unusual, however, is that this domain binds its adjacent proline-rich region at a surface remote from the region previously identified to bind "PxxP" motifs. The interaction may affect the orientation of the tail without sacrificing the availability of the canonical "PxxP"-binding surface.

Keywords: myosin; SH3 domain; PxxP motif; NMR spectroscopy


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