discovery of a gatekeeper residue in the c-terminal tail of the extracellular signal-regulated protein kinase 5 (erk5)

discovery of a gatekeeper residue in the c-terminal tail of the extracellular signal-regulated protein kinase 5 (erk5)

;Adam J. Pearson;Paul Fullwood;Gabriela Toro Tapia;Ian Prise;Michael P. Smith;Qiuping Xu;Allan Jordan;Emanuele Giurisato;Alan J. Whitmarsh;Chiara Francavilla;Cathy Tournier
Intertax 2020 Vol. 21 pp. 929-
336
pearson2020internationaldiscovery

Abstract

The extracellular signal-regulated protein kinase 5 (ERK5) is a non-redundant mitogen-activated protein kinase (MAPK) that exhibits a unique C-terminal extension which comprises distinct structural and functional properties. Here, we sought to elucidate the significance of phosphoacceptor sites in the C-terminal transactivation domain of ERK5. We have found that Thr732 acted as a functional gatekeeper residue controlling C-terminal-mediated nuclear translocation and transcriptional enhancement. Consistently, using a non-bias quantitative mass spectrometry approach, we demonstrated that phosphorylation at Thr732 conferred selectivity for binding interactions of ERK5 with proteins related to chromatin and RNA biology, whereas a number of metabolic regulators were associated with full-length wild type ERK5. Additionally, our proteomic analysis revealed that phosphorylation of the Ser730-Glu-Thr732-Pro motif could occur independently of dual phosphorylation at Thr218-Glu-Tyr220 in the activation loop. Collectively, our results firmly establish the significance of C-terminal phosphorylation in regulating ERK5 function. The post-translational modification of ERK5 on its C-terminal tail might be of particular relevance in cancer cells where ERK5 has be found to be hyperphosphoryated.

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146669
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10.3390/ijms21030929
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