Modeling a disease-correlated tubulin mutation in budding yeast reveals insight into MAP-mediated dynein function

E Denarier,K H Ecklund, G Berthier, A Favier, E T O'Toole, S Gory-Fauré,L De Macedo,C Delphin,A Andrieux,S M Markus,C Boscheron

MOLECULAR BIOLOGY OF THE CELL(2021)

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Abstract
Mutations in the genes that encode alpha- and beta-tubulin underlie many neurological diseases, most notably malformations in cortical development. In addition to revealing the molecular basis for disease etiology, studying such mutations can provide insight into microtubule function and the role of the large family of microtubule effectors. In this study, we use budding yeast to model one such mutation-Gly436Arg in alpha-tubulin, which is causative of malformations in cortical development-in order to understand how it impacts microtubule function in a simple eukaryotic system. Using a combination of in vitro and in vivo methodologies, including live cell imaging and electron tomography, we find that the mutant tubulin is incorporated into microtubules, causes a shift in alpha-tubulin isotype usage, and dramatically enhances dynein activity, which leads to spindle-positioning defects. We find that the basis for the latter phenotype is an impaired interaction between She1-a dynein inhibitor-and the mutant microtubules. In addition to revealing the natural balance of alpha-tubulin isotype utilization in cells, our results provide evidence of an impaired interaction between microtubules and a dynein regulator as a consequence of a tubulin mutation and sheds light on a mechanism that may be causative of neurodevelopmental diseases.
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Key words
tubulin mutation,yeast,disease-correlated,map-mediated
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