Alternative 3′ UTR Selection Controls PAR-5 Homeostasis and Cell Polarity in C. elegans Embryos

•PAR domain size in C. elegans embryos is sensitive to PAR-5 protein levels•PAR-5 protein abundance can be tightly controlled by alternative 3′ UTR selection•SPK-1 regulates par-5 mRNA isoform selection by enhancing 3′ UTR splicing•par-5 3′ UTR selection is essential for the robustness of polarization

SummaryCell polarity in one-cell C. elegans embryos guides asymmetric cell division and cell-fate specification. Shortly after fertilization, embryos establish two antagonistic cortical domains of PAR proteins. Here, we find that the conserved polarity factor PAR-5 regulates PAR domain size in a dose-dependent manner. Using quantitative imaging and controlled genetic manipulation, we find that PAR-5 protein levels reflect the cumulative output of three mRNA isoforms with different translational efficiencies mediated by their 3′ UTRs. 3′ UTR selection is regulated, influencing PAR-5 protein abundance. Alternative splicing underlies the selection of par-5 3′ UTR isoforms. 3′ UTR splicing is enhanced by the SR protein kinase SPK-1, and accordingly, SPK-1 is required for wild-type PAR-5 levels and PAR domain size. Precise regulation of par-5 isoform selection is essential for polarization when the posterior PAR network is compromised. Together, strict control of PAR-5 protein levels and feedback from polarity to par-5 3′ UTR selection confer robustness to embryo polarization.

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