Journal
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
Volume 119, Issue 19, Pages -Publisher
NATL ACAD SCIENCES
DOI: 10.1073/pnas.2122531119
Keywords
protein condensate; condensation phase transition; EGFR; membrane; Ras
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Funding
- NIH National Cancer Institute Physical Sciences in Oncology Network Project [1-U01CA202241]
- Novo Nordisk Foundation Challenge Program under the Center for Geometrically Engineered Cellular Systems
- NIH [PO1 A1091580]
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This study demonstrates that the protein condensation phase transition of EGFR:Grb2 acts as a regulator of signal propagation from EGFR to the MAPK pathway.
We reconstitute a phosphotyrosine-mediated protein condensation phase transition of the similar to 200 residue cytoplasmic tail of the epidermal growth factor receptor (EGFR) and the adaptor protein, Grb2, on a membrane surface. The phase transition depends on phosphorylation of the EGFR tail, which recruits Grb2, and crosslinking through a Grb2-Grb2 binding interface. The Grb2 Y160 residue plays a structurally critical role in the Grb2-Grb2 interaction, and phosphorylation or mutation of Y160 prevents EGFR:Grb2 condensation. By extending the reconstitution experiment to include the guanine nucleotide exchange factor, SOS, and its substrate Ras, we further find that the condensation state of the EGFR tail controls the ability of SOS, recruited via Grb2, to activate Ras. These results identify an EGFR:Grb2 protein condensation phase transition as a regulator of signal propagation from EGFR to the MAPK pathway.
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