Start Over

The SH2 Domain Interaction Landscape

Authors :: Lars Kiemer
Matthias Mann
Nikolaj Blom
Martina Carducci
Luisa Castagnoli
Gianni Cesareni
Stefano Costa
Jesper V. Olsen
Francesca Langone
Kazuya Machida
Christopher M. Thompson
Martin L. Miller
Mike Schutkowski
Michele Tinti
Christopher T. Workman
Søren Brunak
Serena Paoluzi
Francesca Sacco
Bruce J. Mayer
Source :: CELL REPORTS, Cell Reports, Vol 3, Iss 4, Pp 1293-1305 (2013), Tinti, M, Kiemer, L, Costa, S, Miller, M L, Sacco, F, Olsen, J, Carducci, M, Paoluzi, S, Langone, F, Workman, C, Blom, N, Machida, K, Thompson, C M, Schutkowski, M, Brunak, S, Mann, M, Mayer, B J, Castagnoli, L & Cesareni, G 2013, ' The SH2 Domain Interaction Landscape ', Cell Reports, vol. 3, no. 4, pp. 1293-1305 . https://doi.org/10.1016/j.celrep.2013.03.001
Publication Year :: 2013
Publisher :: Elsevier BV, 2013.
Abstract: SummaryMembers of the SH2 domain family modulate signal transduction by binding to short peptides containing phosphorylated tyrosines. Each domain displays a distinct preference for the sequence context of the phosphorylated residue. We have developed a high-density peptide chip technology that allows for probing of the affinity of most SH2 domains for a large fraction of the entire complement of tyrosine phosphopeptides in the human proteome. Using this technique, we have experimentally identified thousands of putative SH2-peptide interactions for more than 70 different SH2 domains. By integrating this rich data set with orthogonal context-specific information, we have assembled an SH2-mediated probabilistic interaction network, which we make available as a community resource in the PepspotDB database. A predicted dynamic interaction between the SH2 domains of the tyrosine phosphatase SHP2 and the phosphorylated tyrosine in the extracellular signal-regulated kinase activation loop was validated by experiments in living cells.