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  • Stress-induced phosphorylation of CLIP-170 by JNK promotes microtubule rescue.

Stress-induced phosphorylation of CLIP-170 by JNK promotes microtubule rescue.

The Journal of cell biology (2020-06-04)
Hélène Henrie, Dalal Bakhos-Douaihy, Isabelle Cantaloube, Antoine Pilon, Maya Talantikite, Virginie Stoppin-Mellet, Anita Baillet, Christian Poüs, Béatrice Benoit
ABSTRACT

The stress-induced c-Jun N-terminal kinase (JNK) controls microtubule dynamics by enhancing both microtubule growth and rescues. Here, we show that upon cell stress, JNK directly phosphorylates the microtubule rescue factor CLIP-170 in its microtubule-binding domain to increase its rescue-promoting activity. Phosphomimetic versions of CLIP-170 enhance its ability to promote rescue events in vitro and in cells. Furthermore, while phosphomimetic mutations do not alter CLIP-170's capability to form comets at growing microtubule ends, both phosphomimetic mutations and JNK activation increase the occurrence of CLIP-170 remnants on the microtubule lattice at the rear of comets. As the CLIP-170 remnants, which are potential sites of microtubule rescue, display a shorter lifetime when CLIP-170 is phosphorylated, we propose that instead of acting at the time of rescue occurrence, CLIP-170 would rather contribute in preparing the microtubule lattice for future rescues at these predetermined sites.

MATERIALS
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Product Description

Sigma-Aldrich
JNK1, active, GST tagged from mouse, PRECISIO® Kinase, recombinant, expressed in baculovirus infected Sf9 cells, ≥90% (SDS-PAGE), buffered aqueous glycerol solution