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Phosphotyrosine-dependent interaction between the kinases PKCθ and Zap70 promotes proximal TCR signaling.

Sci Signal. 2019-04; 
XieJiji,HanXuemei,ZhaoChensi,Canonigo-BalancioAnn J,YatesJohn R,LiYingqiu,LillemeierBj?rn F,AltmanA
Products/Services Used Details Operation
Peptide Synthesis For peptide ELISA, the following N-terminal biotinylated peptides were synthesized and purified to >90% as judged by highperformance liquid chromatography (HPLC) and MS (GenScript): Y126, AMVRDYVRQTWK; pY126, AMVRDpYVRQTWK; Y292, LNSDGYTPEPAR; pY292, LNSDGpYTPEPAR; Y315/319, TSVYESPYSDPE; pY315, TSVpYESPYSDPE; pY319, TSVYESPpYSDPE; and 2pY (pY315 and pY319), TSVpYESPpYSDPE Get A Quote

摘要

Protein kinase C-θ (PKCθ) is an important component of proximal T cell receptor (TCR) signaling. We previously identified the amino-terminal C2 domain of PKCθ as a phosphotyrosine (pTyr)-binding domain. Using a mutant form of PKCθ that cannot bind pTyr (PKCθ), we showed that pTyr binding by PKCθ was required for TCR-induced T cell activation, proliferation, and T2 cell differentiation but not for T cell development. Using tandem mass spectrometry and coimmunoprecipitation, we identified the kinase ζ-associated protein kinase of 70 kDa (Zap70) as a binding partner of the PKCθ pTyr-binding pocket. Tyr of Zap70 directly bound to PKCθ, and the interdomain B residues Tyr and Tyr were indirectly re... More

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