PLoS Genetics (Jun 2022)

A MademoiseLLE domain binding platform links the key RNA transporter to endosomes.

  • Senthil-Kumar Devan,
  • Stephan Schott-Verdugo,
  • Kira Müntjes,
  • Lilli Bismar,
  • Jens Reiners,
  • Eymen Hachani,
  • Lutz Schmitt,
  • Astrid Höppner,
  • Sander Hj Smits,
  • Holger Gohlke,
  • Michael Feldbrügge

DOI
https://doi.org/10.1371/journal.pgen.1010269
Journal volume & issue
Vol. 18, no. 6
p. e1010269

Abstract

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Spatiotemporal expression can be achieved by transport and translation of mRNAs at defined subcellular sites. An emerging mechanism mediating mRNA trafficking is microtubule-dependent co-transport on shuttling endosomes. Although progress has been made in identifying various components of the endosomal mRNA transport machinery, a mechanistic understanding of how these RNA-binding proteins are connected to endosomes is still lacking. Here, we demonstrate that a flexible MademoiseLLE (MLLE) domain platform within RNA-binding protein Rrm4 of Ustilago maydis is crucial for endosomal attachment. Our structure/function analysis uncovered three MLLE domains at the C-terminus of Rrm4 with a functionally defined hierarchy. MLLE3 recognises two PAM2-like sequences of the adaptor protein Upa1 and is essential for endosomal shuttling of Rrm4. MLLE1 and MLLE2 are most likely accessory domains exhibiting a variable binding mode for interaction with currently unknown partners. Thus, endosomal attachment of the mRNA transporter is orchestrated by a sophisticated MLLE domain binding platform.