Genome Biology (Apr 2021)

Drosophila primary microRNA-8 encodes a microRNA-encoded peptide acting in parallel of miR-8

  • Audrey Montigny,
  • Patrizia Tavormina,
  • Carine Duboe,
  • Hélène San Clémente,
  • Marielle Aguilar,
  • Philippe Valenti,
  • Dominique Lauressergues,
  • Jean-Philippe Combier,
  • Serge Plaza

DOI
https://doi.org/10.1186/s13059-021-02345-8
Journal volume & issue
Vol. 22, no. 1
pp. 1 – 21

Abstract

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Abstract Background Recent genome-wide studies of many species reveal the existence of a myriad of RNAs differing in size, coding potential and function. Among these are the long non-coding RNAs, some of them producing functional small peptides via the translation of short ORFs. It now appears that any kind of RNA presumably has a potential to encode small peptides. Accordingly, our team recently discovered that plant primary transcripts of microRNAs (pri-miRs) produce small regulatory peptides (miPEPs) involved in auto-regulatory feedback loops enhancing their cognate microRNA expression which in turn controls plant development. Here we investigate whether this regulatory feedback loop is present in Drosophila melanogaster. Results We perform a survey of ribosome profiling data and reveal that many pri-miRNAs exhibit ribosome translation marks. Focusing on miR-8, we show that pri-miR-8 can produce a miPEP-8. Functional assays performed in Drosophila reveal that miPEP-8 affects development when overexpressed or knocked down. Combining genetic and molecular approaches as well as genome-wide transcriptomic analyses, we show that miR-8 expression is independent of miPEP-8 activity and that miPEP-8 acts in parallel to miR-8 to regulate the expression of hundreds of genes. Conclusion Taken together, these results reveal that several Drosophila pri-miRs exhibit translation potential. Contrasting with the mechanism described in plants, these data shed light on the function of yet undescribed primary-microRNA-encoded peptides in Drosophila and their regulatory potential on genome expression.

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