Nucleotide exchange factor Rab3GEP requires DENN and non-DENN elements for activation and targeting of rab27a

Paolo Sanza, Richard D. Evans, Deborah A. Briggs, Marta Cantero, Lluis Montoliu, Shyamal Patel, Elena V. Sviderskaya, Aymelt Itzen, Ana C. Figueiredo, Miguel C. Seabra, Alistair N. Hume

Research output: Contribution to journalArticlepeer-review

9 Scopus citations

Abstract

Rab GTPases are compartment-specific molecular switches that regulate intracellular vesicular transport in eukaryotes. GDP/GTP exchange factors (GEFs) control Rab activation, and current models propose that localised and regulated GEF activity is important in targeting Rabs to specific membranes. Here, we investigated the mechanism of GEF function using the Rab27a GEF, Rab3GEP (also known as MADD), in melanocytes as a model. We show that Rab3GEP-deficient melanocytes (melan-R3GKO) manifest partial disruption of melanosome dispersion, a read-out of Rab27a activation and targeting. Using rescue of melanosome dispersion in melan-R3GKO cells and effector pull-down approaches we show that the DENN domain of Rab3GEP (conserved among RabGEFs) is necessary, but insufficient, for its cellular function and GEF activity. Finally, using a mitochondrial re-targeting strategy, we show that Rab3GEP can target Rab27a to specific membranes in a GEF-dependent manner. We conclude that Rab3GEP facilitates the activation and targeting of Rab27a to specific membranes, but that it differs from other DENN-containing RabGEFs in requiring DENN and non-DENN elements for both of these activities and by lacking compartment-specific localisation.

Original languageEnglish
Article numberjcs212035
JournalJournal of Cell Science
Volume132
Issue number9
DOIs
StatePublished - 1 May 2019

Keywords

  • Guanine nucleotide exchange factor
  • MADD
  • Melanocyte
  • Organelle transport
  • Rab27a
  • Rab3GEP

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