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<dc:creator>Wei, Qianru</dc:creator>
<dc:creator>Brzostek, Joanna</dc:creator>
<dc:creator>Sankaran, Shvetha</dc:creator>
<dc:creator>Casas Requena, Javier</dc:creator>
<dc:creator>Hew, Lois Shi-Qi</dc:creator>
<dc:creator>Yap, Jiawei</dc:creator>
<dc:creator>Zhao, Xiang</dc:creator>
<dc:creator>Wojciech, Lukasz</dc:creator>
<dc:creator>Gascoigne, Nicholas R. J.</dc:creator>
<dc:date>2020</dc:date>
<dc:description>Producción Científica</dc:description>
<dc:description>Src family kinase Lck plays critical roles during T cell development and activation, as it phosphorylates the TCR/CD3 complex to initiate TCR signaling. Lck is present either in coreceptor-bound or coreceptor-unbound (free) forms, and we here present evidence that the two pools of Lck have different molecular properties. We discovered that the free Lck fraction exhibited higher mobility than CD8α-bound Lck in OT-I T hybridoma cells. The free Lck pool showed more activating Y394 phosphorylation than the coreceptor-bound Lck pool. Consistent with this, free Lck also had higher kinase activity, and free Lck mediated higher T cell activation as compared to coreceptor-bound Lck. Furthermore, the coreceptor-Lck coupling was independent of TCR activation. These findings give insights into the initiation of TCR signaling, suggesting that changes in coreceptor-Lck coupling constitute a mechanism for regulation of T cell sensitivity.</dc:description>
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<dc:language>eng</dc:language>
<dc:title>Lck bound to coreceptor is less active than free Lck</dc:title>
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