The architecture of EGFR's basal complexes reveals autoinhibition mechanisms in dimers and oligomers

Laura C Zanetti-Domingues; Dimitrios Korovesis; Sarah R Needham; Christopher J Tynan; Shiori Sagawa; Selene K Roberts; Antonija Kuzmanic; Elena Ortiz-Zapater; Purvi Jain; Rob C Roovers; Alireza Lajevardipour; Paul M P van Bergen En Henegouwen; George Santis; Andrew H A Clayton; David T Clarke; Francesco L Gervasio; Yibing Shan; David E Shaw; Daniel J Rolfe; Peter J Parker; Marisa L Martin-Fernandez

doi:10.1038/s41467-018-06632-0

The architecture of EGFR's basal complexes reveals autoinhibition mechanisms in dimers and oligomers

Laura C Zanetti-Domingues, Dimitrios Korovesis, Sarah R Needham, Christopher J Tynan, Shiori Sagawa, Selene K Roberts, Antonija Kuzmanic, Elena Ortiz-Zapater, Purvi Jain, Rob C Roovers, Alireza Lajevardipour, Paul M P van Bergen En Henegouwen, George Santis, Andrew H A Clayton, David T Clarke, Francesco L Gervasio, Yibing Shan, David E Shaw, Daniel J Rolfe, Peter J ParkerMarisa L Martin-Fernandez

Central Laser Facility, Research Complex at Harwell, STFC Rutherford Appleton Laboratory, Harwell Oxford, Didcot, Oxford, OX11 0QX, UK.
D. E. Shaw Research, New York, NY, 10036, USA.
Department of Chemistry, Faculty of Maths & Physical Sciences, University College London, London, WC1H 0AJ, UK.
Peter Gore Department of Immunobiology, School of Immunology & Microbial Sciences, Kings College London, London, SE1 9RT, UK.
Centre for Micro-Photonics, Faculty of Science, Engineering and Technology, Swinburne University of Technology, Hawthorn, VIC, 3122, Australia.
Department of Biochemistry and Molecular Biophysics, Columbia University, New York, NY, 10032, USA.
School of Cancer and Pharmaceutical Sciences, King's College London, New Hunt's House, Guy's Campus, London, SE1 1UL, UK.
Central Laser Facility, Research Complex at Harwell, STFC Rutherford Appleton Laboratory, Harwell Oxford, Didcot, Oxford, OX11 0QX, UK. [email protected].
extern

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Our current understanding of epidermal growth factor receptor (EGFR) autoinhibition is based on X-ray structural data of monomer and dimer receptor fragments and does not explain how mutations achieve ligand-independent phosphorylation. Using a repertoire of imaging technologies and simulations we reveal an extracellular head-to-head interaction through which ligand-free receptor polymer chains of various lengths assemble. The architecture of the head-to-head interaction prevents kinase-mediated dimerisation. The latter, afforded by mutation or intracellular treatments, splits the autoinhibited head-to-head polymers to form stalk-to-stalk flexible non-extended dimers structurally coupled across the plasma membrane to active asymmetric tyrosine kinase dimers, and extended dimers coupled to inactive symmetric kinase dimers. Contrary to the previously proposed main autoinhibitory function of the inactive symmetric kinase dimer, our data suggest that only dysregulated species bear populations of symmetric and asymmetric kinase dimers that coexist in equilibrium at the plasma membrane under the modulation of the C-terminal domain.

Original language	English
Article number	4325
Journal	Nature Communications
Volume	9
Issue number	1
DOIs	https://doi.org/10.1038/s41467-018-06632-0
Publication status	Published - 18 Oct 2018

Keywords

Animals
CHO Cells
Cell Membrane/metabolism
Cricetinae
Cricetulus
ErbB Receptors/antagonists & inhibitors
Extracellular Matrix/metabolism
Fluorescent Dyes/chemistry
Ligands
Models, Biological
Models, Molecular
Photobleaching
Polymers/chemistry
Protein Domains
Protein Kinases/chemistry
Protein Multimerization

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Zanetti-Domingues, L. C., Korovesis, D., Needham, S. R., Tynan, C. J., Sagawa, S., Roberts, S. K., Kuzmanic, A., Ortiz-Zapater, E., Jain, P., Roovers, R. C., Lajevardipour, A., van Bergen En Henegouwen, P. M. P., Santis, G., Clayton, A. H. A., Clarke, D. T., Gervasio, F. L., Shan, Y., Shaw, D. E., Rolfe, D. J., ... Martin-Fernandez, M. L. (2018). The architecture of EGFR's basal complexes reveals autoinhibition mechanisms in dimers and oligomers. Nature Communications, 9(1), Article 4325. https://doi.org/10.1038/s41467-018-06632-0

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title = "The architecture of EGFR's basal complexes reveals autoinhibition mechanisms in dimers and oligomers",

abstract = "Our current understanding of epidermal growth factor receptor (EGFR) autoinhibition is based on X-ray structural data of monomer and dimer receptor fragments and does not explain how mutations achieve ligand-independent phosphorylation. Using a repertoire of imaging technologies and simulations we reveal an extracellular head-to-head interaction through which ligand-free receptor polymer chains of various lengths assemble. The architecture of the head-to-head interaction prevents kinase-mediated dimerisation. The latter, afforded by mutation or intracellular treatments, splits the autoinhibited head-to-head polymers to form stalk-to-stalk flexible non-extended dimers structurally coupled across the plasma membrane to active asymmetric tyrosine kinase dimers, and extended dimers coupled to inactive symmetric kinase dimers. Contrary to the previously proposed main autoinhibitory function of the inactive symmetric kinase dimer, our data suggest that only dysregulated species bear populations of symmetric and asymmetric kinase dimers that coexist in equilibrium at the plasma membrane under the modulation of the C-terminal domain.",

keywords = "Animals, CHO Cells, Cell Membrane/metabolism, Cricetinae, Cricetulus, ErbB Receptors/antagonists \& inhibitors, Extracellular Matrix/metabolism, Fluorescent Dyes/chemistry, Ligands, Models, Biological, Models, Molecular, Photobleaching, Polymers/chemistry, Protein Domains, Protein Kinases/chemistry, Protein Multimerization",

author = "Zanetti-Domingues, \{Laura C\} and Dimitrios Korovesis and Needham, \{Sarah R\} and Tynan, \{Christopher J\} and Shiori Sagawa and Roberts, \{Selene K\} and Antonija Kuzmanic and Elena Ortiz-Zapater and Purvi Jain and Roovers, \{Rob C\} and Alireza Lajevardipour and \{van Bergen En Henegouwen\}, \{Paul M P\} and George Santis and Clayton, \{Andrew H A\} and Clarke, \{David T\} and Gervasio, \{Francesco L\} and Yibing Shan and Shaw, \{David E\} and Rolfe, \{Daniel J\} and Parker, \{Peter J\} and Martin-Fernandez, \{Marisa L\}",

year = "2018",

month = oct,

day = "18",

doi = "10.1038/s41467-018-06632-0",

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Zanetti-Domingues, LC, Korovesis, D, Needham, SR, Tynan, CJ, Sagawa, S, Roberts, SK, Kuzmanic, A, Ortiz-Zapater, E, Jain, P, Roovers, RC, Lajevardipour, A, van Bergen En Henegouwen, PMP, Santis, G, Clayton, AHA, Clarke, DT, Gervasio, FL, Shan, Y, Shaw, DE, Rolfe, DJ, Parker, PJ & Martin-Fernandez, ML 2018, 'The architecture of EGFR's basal complexes reveals autoinhibition mechanisms in dimers and oligomers', Nature Communications, vol. 9, no. 1, 4325. https://doi.org/10.1038/s41467-018-06632-0

TY - JOUR

T1 - The architecture of EGFR's basal complexes reveals autoinhibition mechanisms in dimers and oligomers

AU - Zanetti-Domingues, Laura C

AU - Korovesis, Dimitrios

AU - Needham, Sarah R

AU - Tynan, Christopher J

AU - Sagawa, Shiori

AU - Roberts, Selene K

AU - Kuzmanic, Antonija

AU - Ortiz-Zapater, Elena

AU - Jain, Purvi

AU - Roovers, Rob C

AU - Lajevardipour, Alireza

AU - van Bergen En Henegouwen, Paul M P

AU - Santis, George

AU - Clayton, Andrew H A

AU - Clarke, David T

AU - Gervasio, Francesco L

AU - Shan, Yibing

AU - Shaw, David E

AU - Rolfe, Daniel J

AU - Parker, Peter J

AU - Martin-Fernandez, Marisa L

PY - 2018/10/18

Y1 - 2018/10/18

N2 - Our current understanding of epidermal growth factor receptor (EGFR) autoinhibition is based on X-ray structural data of monomer and dimer receptor fragments and does not explain how mutations achieve ligand-independent phosphorylation. Using a repertoire of imaging technologies and simulations we reveal an extracellular head-to-head interaction through which ligand-free receptor polymer chains of various lengths assemble. The architecture of the head-to-head interaction prevents kinase-mediated dimerisation. The latter, afforded by mutation or intracellular treatments, splits the autoinhibited head-to-head polymers to form stalk-to-stalk flexible non-extended dimers structurally coupled across the plasma membrane to active asymmetric tyrosine kinase dimers, and extended dimers coupled to inactive symmetric kinase dimers. Contrary to the previously proposed main autoinhibitory function of the inactive symmetric kinase dimer, our data suggest that only dysregulated species bear populations of symmetric and asymmetric kinase dimers that coexist in equilibrium at the plasma membrane under the modulation of the C-terminal domain.

AB - Our current understanding of epidermal growth factor receptor (EGFR) autoinhibition is based on X-ray structural data of monomer and dimer receptor fragments and does not explain how mutations achieve ligand-independent phosphorylation. Using a repertoire of imaging technologies and simulations we reveal an extracellular head-to-head interaction through which ligand-free receptor polymer chains of various lengths assemble. The architecture of the head-to-head interaction prevents kinase-mediated dimerisation. The latter, afforded by mutation or intracellular treatments, splits the autoinhibited head-to-head polymers to form stalk-to-stalk flexible non-extended dimers structurally coupled across the plasma membrane to active asymmetric tyrosine kinase dimers, and extended dimers coupled to inactive symmetric kinase dimers. Contrary to the previously proposed main autoinhibitory function of the inactive symmetric kinase dimer, our data suggest that only dysregulated species bear populations of symmetric and asymmetric kinase dimers that coexist in equilibrium at the plasma membrane under the modulation of the C-terminal domain.

KW - Animals

KW - CHO Cells

KW - Cell Membrane/metabolism

KW - Cricetinae

KW - Cricetulus

KW - ErbB Receptors/antagonists & inhibitors

KW - Extracellular Matrix/metabolism

KW - Fluorescent Dyes/chemistry

KW - Ligands

KW - Models, Biological

KW - Models, Molecular

KW - Photobleaching

KW - Polymers/chemistry

KW - Protein Domains

KW - Protein Kinases/chemistry

KW - Protein Multimerization

U2 - 10.1038/s41467-018-06632-0

DO - 10.1038/s41467-018-06632-0

M3 - Article

C2 - 30337523

SN - 2041-1723

VL - 9

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 4325

ER -

The architecture of EGFR's basal complexes reveals autoinhibition mechanisms in dimers and oligomers

Abstract

Keywords

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