Reticulon-1 synthesis controls outgrowth and microtubule dynamics in injured cortical axons

  • Alejandro Luarte
  • , Javiera Gallardo
  • , Daniela Corvalán
  • , Ankush Chakraborty
  • , Cláudio Gouveia Roque
  • , Francisca Bertin
  • , Carlos Contreras
  • , Juan Pablo Ramírez
  • , André Weber
  • , Waldo Acevedo
  • , Werner Zuschratter
  • , Rodrigo Herrera-Molina
  • , Úrsula Wyneken
  • , Andrea Paula-Lima
  • , Tatiana Adasme-Rocha
  • , Jorge Toledo
  • , Rodrigo Vergara
  • , Antonia Figueroa
  • , Carolina González
  • , Christian González-Billault
  • Ulrich Hengst, Andrés Couve

Research output: Contribution to journalArticlepeer-review

Abstract

The regenerative potential of developing cortical axons depends on intrinsic mechanisms, such as axon-autonomous protein synthesis, that are still not fully understood. An emerging factor in this regenerative response is the bidirectional interplay between microtubule dynamics and the axonal ER. We hypothesize that locally synthesized ER proteins regulate microtubule dynamics and the regeneration of cortical axons. RNA data mining identified the ER-shaping protein Reticulon-1 as a relevant candidate across eight axonal transcriptomes. Using microfluidics, we show that axonal treatment with a small RNA against Reticulon-1 mRNA (Reticulon-1 knockdown) increases outgrowth of injured cortical axons while reducing their tubulin levels. We show by live-cell imaging that axonal Reticulon-1 knockdown increases microtubule growth rate in noninjured axons and restores this parameter after injury. Axonal inhibition of the microtubule-severing protein Spastin prevents the effects of Reticulon-1 knockdown over tubulin levels and outgrowth. We provide evidence that the Reticulon-1C isoform is synthesized within axons and attenuates Spastin-mediated microtubule severing. These findings support a model in which axonal protein synthesis regulates microtubule dynamics and axon outgrowth after injury.

Original languageEnglish
JournalLife Science Alliance
Volume9
Issue number4
DOIs
StatePublished - 1 Apr 2026

Bibliographical note

© 2026 Luarte et al.

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