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Aurora A site specific TACC3 phosphorylation regulates astral microtubule assembly by stabilizing γ-tubulin ring complex.

Authors :
Rajeev, Resmi
Singh, Puja
Asmita, Ananya
Anand, Ushma
Manna, Tapas K.
Source :
BMC Molecular & Cell Biology. 12/10/2019, p1-13. 13p.
Publication Year :
2019

Abstract

Background: Astral microtubules emanating from the mitotic centrosomes play pivotal roles in defining cell division axis and tissue morphogenesis. Previous studies have demonstrated that human transforming acidic coiledcoil 3 (TACC3), the most conserved TACC family protein, regulates formation of astral microtubules at centrosomes in vertebrate cells by affecting γ-tubulin ring complex (γ-TuRC) assembly. However, the molecular mechanisms underlying such function were not completely understood. Results: Here, we show that Aurora A site-specific phosphorylation in TACC3 regulates formation of astral microtubules by stabilizing γ-TuRC assembly in human cells. Mutation of the most conserved Aurora A targeting site, Ser 558 to alanine (S558A) in TACC3 results in robust loss of astral microtubules and disrupts localization of the γ-tubulin ring complex (γ-TuRC) proteins at the spindle poles. Under similar condition, phospho-mimicking S558D mutation retains astral microtubules and the γ-TuRC proteins in a manner similar to control cells expressed with wild type TACC3. Time-lapse imaging reveals that S558A mutation leads to defects in positioning of the spindlepoles and thereby causes delay in metaphase to anaphase transition. Biochemical results determine that the Ser 558-phosphorylated TACC3 interacts with the γ-TuRC proteins and further, S558A mutation impairs the interaction. We further reveal that the mutation affects the assembly of γ-TuRC from the small complex components. Conclusions: The results demonstrate that TACC3 phosphorylation stabilizes γ-tubulin ring complex assembly and thereby regulates formation of centrosomal asters. They also implicate a potential role of TACC3 phosphorylation in the functional integrity of centrosomes/spindle poles. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
26618850
Database :
Academic Search Index
Journal :
BMC Molecular & Cell Biology
Publication Type :
Academic Journal
Accession number :
143751170
Full Text :
https://doi.org/10.1186/s12860-019-0242-z