Myosin-X is dispensable for spindle morphogenesis and positioning in the mouse oocyte

Author:

Crozet Flora1,Da Silva Christelle1,Verlhac Marie-Hélène1ORCID,Terret Marie-Emilie1ORCID

Affiliation:

1. CIRB, Collège de France, UMR7241/U1050, 75005 Paris, France

Abstract

ABSTRACT Off-center spindle positioning in mammalian oocytes enables asymmetric divisions in size, which are important for subsequent embryogenesis. The migration of the meiosis I spindle from the oocyte center to its cortex is mediated by F-actin. Specifically, an F-actin cage surrounds the microtubule spindle and applies forces to it. To better understand how F-actin transmits forces to the spindle, we studied a potential direct link between F-actin and microtubules. For this, we tested the implication of myosin-X, a known F-actin and microtubule binder involved in spindle morphogenesis and/or positioning in somatic cells, amphibian oocytes and embryos. Using a mouse strain conditionally invalidated for myosin-X in oocytes and by live-cell imaging, we show that myosin-X is not localized on the spindle, and is dispensable for spindle and F-actin assembly. It is not required for force transmission as spindle migration and chromosome alignment occur normally. More broadly, myosin-X is dispensable for oocyte developmental potential and female fertility. We therefore exclude a role for myosin-X in transmitting F-actin-mediated forces to the spindle, opening new perspectives regarding this mechanism in mouse oocytes, which differ from most mitotic cells.

Funder

Agence Nationale de la Recherche

France Canada Research Fund

Fondation pour la Recherche Médicale

Fondation Bettencourt Schueller

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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