Developmental Cell
Volume 37, Issue 6, 20 June 2016, Pages 507-519
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Article
Stuxnet Facilitates the Degradation of Polycomb Protein during Development

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Highlights

  • Stuxnet (Stx) and Polycomb (Pc) proteins display reciprocal expression patterns

  • Stx facilitates Pc protein degradation through a ubiquitin-independent pathway

  • Stx modulates PRC1 activity to epigenetically control target gene transcription

  • Stx effect on Pc is conserved from flies to vertebrates

Summary

Polycomb-group (PcG) proteins function to ensure correct deployment of developmental programs by epigenetically repressing target gene expression. Despite the importance, few studies have been focused on the regulation of PcG activity itself. Here, we report a Drosophila gene, stuxnet (stx), that controls Pc protein stability. We find that heightened stx activity leads to homeotic transformation, reduced Pc activity, and de-repression of PcG targets. Conversely, stx mutants, which can be rescued by decreased Pc expression, display developmental defects resembling hyperactivation of Pc. Our biochemical analyses provide a mechanistic basis for the interaction between stx and Pc; Stx facilitates Pc degradation in the proteasome, independent of ubiquitin modification. Furthermore, this mode of regulation is conserved in vertebrates. Mouse stx promotes degradation of Cbx4, an orthologous Pc protein, in vertebrate cells and induces homeotic transformation in Drosophila. Our results highlight an evolutionarily conserved mechanism of regulated protein degradation on PcG homeostasis and epigenetic activity.

Cited by (0)

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Co-first author

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Present address: Department of Entomology, China Agricultural University, Beijing 100193, China

6

Present address: Institute of Evolution and Marine Biodiversity, Ocean University of China, Qingdao 266003, China