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Backbone nuclear relaxation characteristics and calorimetric investigation of the human Grb7-SH2/erbB2 peptide complex
Authors:Ivancic Monika  Spuches Anne M  Guth Ethan C  Daugherty Margaret A  Wilcox Dean E  Lyons Barbara A
Institution:Department of Biochemistry, College of Medicine, University of Vermont, Burlington 05405, USA.
Abstract:Grb7 is a member of the Grb7 family of proteins, which also includes Grb10 and Grb14. All three proteins have been found to be overexpressed in certain cancers and cancer cell lines. In particular, Grb7 (along with the receptor tyrosine kinase erbB2) is overexpressed in 20%–30% of breast cancers. Grb7 binds to erbB2 and may be involved in cell signaling pathways that promote the formation of metastases and inflammatory responses. In a prior study, we reported the solution structure of the Grb7-SH2/erbB2 peptide complex. In this study, T1, T2, and steady-state NOE measurements were performed on the Grb7-SH2 domain, and the backbone relaxation behavior of the domain is discussed with respect to the potential function of an insert region present in all three members of this protein family. Isothermal titration calorimetry (ITC) studies were completed measuring the thermodynamic parameters of the binding of a 10-residue phosphorylated peptide representative of erbB2 to the SH2 domain. These measurements are compared to calorimetric studies performed on other SH2 domain/phosphorylated peptide complexes available in the literature.
Keywords:BPS  between Plekstrin and Src  EGFR  epidermal growth factor receptor  erbB2 (aka HER2  EGFR2)  erythroblastosis B  FGFR  fibroblast growth factor receptor  Grb  growth factor receptor bound  HSQC  heteronuclear single‐quantum coherence  J(ω)  spectral density function  IR  insulin receptor  ITC  isothermal titration calorimetry  NMR  nuclear magnetic resonance  NOE  nuclear Overhauser effect  NOESY  NOE spectroscopy  PDGFR  platelet derived growth factor receptor  T1  longitudinal relaxation time (aka spin‐lattice)  T2  transverse relaxation time (aka spin–spin)  τm  molecular correlation time  τe  effective correlation time  RMSD  root‐mean‐square deviation  RTK  receptor tyrosine kinase  S2  order parameter  SH2  Src homology 2  
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