HOOK2 mediates dynein-dynactin association to regulate mitotic progression and cytokinesis
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Abstract
Hook proteins are evolutionarily conserved dynein adaptors that promote assembly of highly
processive dynein-dynactin motor complexes. Mammals contain three Hook paralogs, namely
Hook1, Hook2 and Hook3 that have distinct subcellular localisations and expectedly, distinct
cellular functions. Here we demonstrate that Hook2 binds to, and promotes dynein-dynactin
assembly specifically during mitosis. During the late G2 phase, Hook2 mediates dynein-dynactin
localization at the nuclear envelope (NE), which is required for centrosome anchoring to the NE.
Independent of its binding to dynein, Hook2 regulates microtubule nucleation at the centrosome-
accordingly, Hook2-depleted cells have reduced astral microtubules and spindle positioning
defects. Besides the centrosome, Hook2 localizes to, and recruits dynactin and dynein to the
central spindle. Dynactin-dependent targeting of centralspindlin complex to the midzone is
abrogated upon Hook2 depletion, accordingly Hook2 depletion results in cytokinesis failure. We
find that the zebrafish Hook2 homolog promotes dynein-dynactin association and was essential
for zebrafish early development. Together, these results suggest that Hook2 mediates assembly of
the dynein-dynactin complex and regulates mitotic progression and cytokinesis.