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Molecular principles of Piwi-mediated cotranscriptional silencing through the dimeric SFiNX complex.

Jakob SchnablJuncheng WangUlrich HohmannMaja GehreJulia BatkiVeselin I AndreevKim PurkhauserNina FaschingPeter DuchekMaria NovatchkovaKarl MechtlerClemens PlaschkaDinshaw J PatelJulius Brennecke
Published in: Genes & development (2021)
Nuclear Argonaute proteins, guided by their bound small RNAs to nascent target transcripts, mediate cotranscriptional silencing of transposons and repetitive genomic loci through heterochromatin formation. The molecular mechanisms involved in this process are incompletely understood. Here, we show that the SFiNX complex, a silencing mediator downstream from nuclear Piwi-piRNA complexes in Drosophila, facilitates cotranscriptional silencing as a homodimer. The dynein light chain protein Cut up/LC8 mediates SFiNX dimerization, and its function can be bypassed by a heterologous dimerization domain, arguing for a constitutive SFiNX dimer. Dimeric, but not monomeric SFiNX, is capable of forming molecular condensates in a nucleic acid-stimulated manner. Mutations that prevent SFiNX dimerization result in loss of condensate formation in vitro and the inability of Piwi to initiate heterochromatin formation and silence transposons in vivo. We propose that multivalent SFiNX-nucleic acid interactions are critical for heterochromatin establishment at piRNA target loci in a cotranscriptional manner.
Keyphrases
  • nucleic acid
  • genome wide
  • high frequency
  • single molecule
  • small molecule
  • gene expression
  • genome wide association study
  • mass spectrometry
  • copy number
  • binding protein
  • genome wide association
  • bacillus subtilis