Abstract

Tec family tyrosine kinases transduce signals from antigen and other receptors. In particular, Itk plays an important role in T-cell development and activation. Itk has an N-terminal pleckstrin homology domain, a Tec Homology domain with a proline-rich region, SH3 and SH2 domains and a kinase domain, the structure each of which has been determined. However, the full structure of Itk and other Tec kinases remain elusive. Models of Itk suggest either a head to tail dimer, with the SH2 domain interacting with the SH3 domain, or a folded monomer with the SH3 domain interacting with the proline-rich region. We show here that in vivo Itk exists as a monomer, with the pleckstrin homology domain less than 80 A from the C terminus. Zn2+ coordinating residues in the Tec Homology domain, not the proline-rich region, are critical for this intramolecular interaction. These data have implications for our understanding of Tec family kinase structure.

Highlights

  • The Tec family of non-receptor tyrosine kinases, including Itk,2 is the second largest family of non-receptor tyrosine kinases [1]

  • We show here that in vivo Itk exists as a monomer, with the pleckstrin homology domain less than 80 Afrom the C terminus

  • 2 The abbreviations used are: Itk, inducible T cell kinase; PH, pleckstrin homology domain; BcR, B cell receptor; BH, Btk homology domain; CypA, cyclophilin A; ECFP, enhanced cyan fluorescent protein; GFP, green fluorescent protein; PRR, proline-rich region; TcR, T cell receptor; TH, Tec homology domain; SH2, Src homology domain 2; SH3, Src homology domain 3; YFP, yellow fluorescent protein; Y1I, YFP1 fragment tagged to Itk; Y2I, YFP2 fragment tagged to Itk; FRET, fluorescence resonance energy transfer; WT, wild type

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Summary

Introduction

The Tec family of non-receptor tyrosine kinases, including Itk,2 is the second largest family of non-receptor tyrosine kinases [1].

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