Abstract
In non-motile fungi, sexual reproduction relies on strong morphogenetic changes in response to pheromone signaling. We report here on a systematic screen for morphological abnormalities of the mating process in fission yeast Schizosaccharomyces pombe. We derived a homothallic (self-fertile) collection of viable deletions, which, upon visual screening, revealed a plethora of phenotypes affecting all stages of the mating process, including cell polarization, cell fusion and sporulation. Cell fusion relies on the formation of the fusion focus, an aster-like F-actin structure that is marked by strong local accumulation of the myosin V Myo52, which concentrates secretion at the fusion site. A secondary screen for fusion-defective mutants identified the myosin V Myo51-associated coiled-coil proteins Rng8 and Rng9 as critical for the coalescence of the fusion focus. Indeed, rng8Δ and rng9Δ mutant cells exhibit multiple stable dots at the cell-cell contact site, instead of the single focus observed in wildtype. Rng8 and Rng9 accumulate on the fusion focus, dependent on Myo51 and tropomyosin Cdc8. A tropomyosin mutant allele, which compromises Rng8/9 localization but not actin binding, similarly leads to multiple stable dots instead of a single focus. By contrast, myo51 deletion does not strongly affect fusion focus coalescence. We propose that focusing of the actin filaments in the fusion aster primarily relies on Rng8/9-dependent cross-linking of tropomyosin-actin filaments.
Highlights
Sexual reproduction is carried out by most eukaryotes and permits the alternation of haploid and diploid life stages
We report on a systematic screen for mutants with morphological abnormalities during sexual reproduction in the fission yeast, Schizosaccharomyces pombe, a widely used model for the study of fundamental cellular processes
It relies on the formation of differentiated haploid cell types that are able to meet and fuse to form a zygote, which eventually returns to the haploid state through meiosis
Summary
Sexual reproduction is carried out by most eukaryotes and permits the alternation of haploid and diploid life stages. It relies on the formation of differentiated haploid cell types that are able to meet and fuse to form a zygote, which eventually returns to the haploid state through meiosis. We have used the fission yeast Schizosaccharomyces pombe to systematically screen for viable gene deletions causing a morphological abnormality in the sexual reproduction process. We anticipated this screen would shed light on the processes of cell polarization, cell-cell fusion and sporulation
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