zyg-11 and cul-2 regulate progression through meiosis II and polarity establishment in C. elegans

doi:10.1242/dev.01244

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First published online 23 June 2004
doi: 10.1242/dev.01244

Development 131, 3527-3543 (2004)
Published by The Company of Biologists 2004

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zyg-11 and cul-2 regulate progression through meiosis II and polarity establishment in C. elegans

Rémi Sonneville and Pierre Gönczy^*

ISREC (Swiss Institute for Experimental Cancer Research), 155, chemin des Boveresses, CH-1066 Epalinges/Lausanne, Switzerland

^* Author for correspondence (e-mail: pierre.gonczy{at}isrec.unil.ch)

Accepted 30 April 2004

The mechanisms that ensure coupling between meiotic cell cycleprogression and subsequent developmental events, including specificationof embryonic axes, are poorly understood. Here, we establishthat zyg-11 and the cullin cul-2 promote the metaphase-to-anaphasetransition and M phase exit at meiosis II in Caenorhabditiselegans. Our results indicate that ZYG-11 acts with a CUL-2-basedE3 ligase that is essential at meiosis II and that functionsredundantly with the anaphase-promoting complex/cyclosome atmeiosis I. Our data also indicate that delayed M phase exitin zyg-11(RNAi) embryos is due to accumulation of the B type cyclinCYB-3. We demonstrate that PAR proteins and P granules becomepolarized in an inverted manner during the meiosis II delayresulting from zyg-11 or cul-2 inactivation, and that zyg-11and cul-2 can regulate polarity establishment independentlyof a role in cell cycle progression. Furthermore, we find thatmicrotubules appear dispensable for ectopic polarity duringthe meiosis II delay in zyg-11(RNAi) embryos, as well as forAP polarity during the first mitotic cell cycle in wild-typeembryos. Our findings suggest a model in which a CUL-2-basedE3 ligase promotes cell cycle progression and prevents polarityestablishment during meiosis II, and in which the centrosomeacts as a cue to polarize the embryo along the AP axis afterexit from the meiotic cell cycle.

Key words: Meiotic cell cycle, AP polarity, E3 ligase, C. elegans, APC

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