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CD and NMR conformational studies of a peptide encompassing the Mid Loop interface of Ship2–Sam
Authors:Concetta Di Natale  Daniela Marasco  Maurizio Pellecchia  Marilisa Leone
Institution:1. Department of Pharmacy, University "Federico II", Naples, Italy;2. IIT Italian Institute of Technology, Naples, Italy;3. Institute of Biostructures and Bioimaging (CNR), Naples, Italy;4. Centro Interuniversitario di Ricerca sui Peptidi Bioattivi (CIRPEB), Naples, Italy;5. Sanford‐Burnham Medical Research Institute, La Jolla, CA
Abstract:The lipid phosphatase Ship2 is a protein that intervenes in several diseases such as diabetes, cancer, neurodegeneration, and atherosclerosis. It is made up of a catalytic domain and several protein docking modules such as a C‐terminal Sam (Sterile alpha motif) domain. The Sam domain of Ship2 (Ship2–Sam) binds to the Sam domains of the EphA2 receptor (EphA2–Sam) and the PI3K effector protein Arap3 (Arap3–Sam). These heterotypic Sam–Sam interactions occur through formation of dimers presenting the canonical “Mid Loop/End Helix” binding mode. The central region of Ship2–Sam, spanning the C‐terminal end of α2, the α3 and α4 helices together with the α2α3 and α3α4 interhelical loops, forms the Mid Loop surface that is needed to bind partners Sam domains. A peptide encompassing most of the Ship2–Sam Mid Loop interface (Shiptide) capable of binding to both EphA2–Sam and Arap3–Sam, was previously identified. Here we investigated the conformational features of this peptide, through solution CD and NMR studies in different conditions. These studies reveal that the peptide is highly flexible in aqueous buffer, while it adopts a helical conformation in presence of 2,2,2‐trifluoroethanol. The discovered structural insights and in particular the identification of a helical motif, may lead to the design of more constrained and possibly cell permeable Shiptide analogs that could work as efficient antagonists of Ship2–Sam heterotypic interactions and embrace therapeutic applications. © 2014 Wiley Periodicals, Inc. Biopolymers 101: 1088–1098, 2014.
Keywords:Sam domain  Ship2  peptide  NMR  CD
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