Affiliation:
1. Department of Molecular Medicine, Institute of Basic Medical Sciences University of Oslo Oslo Norway
Abstract
AbstractAdapter proteins are flexible and dynamic modulators of cellular signalling that are important for immune cell function. One of these, the T‐cell‐specific adapter protein (TSAd), interacts with the non‐receptor tyrosine kinases Src and Lck of the Src family kinases (SFKs) and Itk of the Tec family kinases (TFKs). Three tyrosine residues in the TSAd C‐terminus are phosphorylated by Lck and serve as docking sites for the Src homology 2 (SH2) domains of Src and Lck. The TSAd proline‐rich region (PRR) binds to the Src homology 3 (SH3) domains found in Lck, Src and Itk. Despite known interactors, the role TSAd plays in cellular signalling remains largely unknown. TSAd's ability to bind both SFKs and TFKs may point to its function as a general scaffold for both kinase families. Using GST‐pulldown as well as peptide array experiments, we found that both the SH2 and SH3 domains of the SFKs Fyn and Hck, as well as the TFKs Tec and Txk, interact with TSAd. This contrasts with Itk, which interacts with TSAd only through its SH3 domain. Although our analysis showed that TSAd is both co‐expressed and may interact with Fyn, we were unable to co‐precipitate Fyn with TSAd from Jurkat cells, as detected by Western blotting and affinity purification mass spectrometry. This may suggest that TSAd‐Fyn interaction in intact cells may be limited by other factors, such as the subcellular localization of the two molecules or the co‐expression of competing binding partners.
Funder
Universitetet i Oslo
Anders Jahres Fond til Vitenskapens Fremme
Cited by
1 articles.
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