1. Academic Validation
  2. EGFR-RAS-MAPK signaling is confined to the plasma membrane and associated endorecycling protrusions

EGFR-RAS-MAPK signaling is confined to the plasma membrane and associated endorecycling protrusions

  • J Cell Biol. 2021 Nov 1;220(11):e202107103. doi: 10.1083/jcb.202107103.
Sachin Surve 1 Simon C Watkins 1 Alexander Sorkin 1
Affiliations

Affiliation

  • 1 Department of Cell Biology, University of Pittsburgh School of Medicine, Pittsburgh, PA.
Abstract

The subcellular localization of Ras GTPases defines the operational compartment of the EGFR-ERK1/2 signaling pathway within cells. Hence, we used live-cell imaging to demonstrate that endogenous KRAS and NRAS tagged with mNeonGreen are predominantly localized to the plasma membrane. NRAS was also present in the Golgi apparatus and a tubular, plasma-membrane derived endorecycling compartment, enriched in recycling endosome markers (TERC). In EGF-stimulated cells, there was essentially no colocalization of either mNeonGreen-KRAS or mNeonGreen-NRAS with endosomal EGFR, which, by contrast, remained associated with endogenous Grb2-mNeonGreen, a receptor adaptor upstream of Ras. ERK1/2 activity was diminished by blocking cell surface EGFR with cetuximab, even after most ligand-bound, Grb2-associated EGFRs were internalized. Endogenous mCherry-tagged RAF1, an effector of Ras, was recruited to the plasma membrane, with subsequent accumulation in mNG-NRAS-containing TERCs. We propose that a small pool of surface EGFRs sustain signaling within the RAS-ERK1/2 pathway and that Ras activation persists in TERCs, whereas endosomal EGFR does not significantly contribute to ERK1/2 activity.

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