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PDBsum entry 1gl5
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Contents |
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* Residue conservation analysis
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References listed in PDB file
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Key reference
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Title
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The solution structure and intramolecular associations of the tec kinase src homology 3 domain.
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Authors
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S.E.Pursglove,
T.D.Mulhern,
J.P.Mackay,
M.G.Hinds,
G.W.Booker.
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Ref.
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J Biol Chem, 2002,
277,
755-762.
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PubMed id
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Abstract
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Tec is the prototypic member of a family of intracellular tyrosine kinases that
includes Txk, Bmx, Itk, and Btk. Tec family kinases share similarities in domain
structure with Src family kinases, but one of the features that differentiates
them is a proline-rich region (PRR) preceding their Src homology (SH) 3 domain.
Evidence that the PRR of Itk can bind in an intramolecular fashion to its SH3
domain and the lack of a regulatory tyrosine in the C terminus indicates that
Tec kinases must be regulated by a different set of intramolecular interactions
to the Src kinases. We have determined the solution structure of the Tec SH3
domain and have investigated interactions with its PRR, which contains two
SH3-binding sites. We demonstrate that in vitro, the Tec PRR can bind in an
intramolecular fashion to the SH3. However, the affinity is lower than that for
dimerization via reciprocal PRR-SH3 association. Using site-directed mutagenesis
we show that both sites can bind the Tec SH3 domain; site 1 (155KTLPPAP161)
binds intramolecularly, while site 2 (165KRRPPPPIPP174) cannot and binds in an
intermolecular fashion. These distinct roles for the SH3 binding sites in Tec
family kinases could be important for protein targeting and enzyme activation.
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