[HTML][HTML] Aurora A drives early signalling and vesicle dynamics during T-cell activation

N Blas-Rus, E Bustos-Morán, I Pérez de Castro… - Nature …, 2016 - nature.com
N Blas-Rus, E Bustos-Morán, I Pérez de Castro, G De Cárcer, A Borroto, E Camafeita
Nature communications, 2016nature.com
Aurora A is a serine/threonine kinase that contributes to the progression of mitosis by
inducing microtubule nucleation. Here we have identified an unexpected role for Aurora A
kinase in antigen-driven T-cell activation. We find that Aurora A is phosphorylated at the
immunological synapse (IS) during TCR-driven cell contact. Inhibition of Aurora A with
pharmacological agents or genetic deletion in human or mouse T cells severely disrupts the
dynamics of microtubules and CD3ζ-bearing vesicles at the IS. The absence of Aurora A …
Abstract
Aurora A is a serine/threonine kinase that contributes to the progression of mitosis by inducing microtubule nucleation. Here we have identified an unexpected role for Aurora A kinase in antigen-driven T-cell activation. We find that Aurora A is phosphorylated at the immunological synapse (IS) during TCR-driven cell contact. Inhibition of Aurora A with pharmacological agents or genetic deletion in human or mouse T cells severely disrupts the dynamics of microtubules and CD3ζ-bearing vesicles at the IS. The absence of Aurora A activity also impairs the activation of early signalling molecules downstream of the TCR and the expression of IL-2, CD25 and CD69. Aurora A inhibition causes delocalized clustering of Lck at the IS and decreases phosphorylation levels of tyrosine kinase Lck, thus indicating Aurora A is required for maintaining Lck active. These findings implicate Aurora A in the propagation of the TCR activation signal.
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