PKCθ links proximal T cell and notch signaling through localized regulation of the actin cytoskeleton

Graham J. Britton; Rachel Ambler; Danielle J. Clark; Elaine V. Hill; Helen M. Tunbridge; Kerrie E. McNally; Bronwen R. Burton; Philomena Butterweck; Catherine Sabatos-Peyton; Lea A. Hampton-O’neil; Paul Verkade; Christoph Wuelfing; David Cameron Wraith

doi:10.7554/eLife.20003

PKCθ links proximal T cell and notch signaling through localized regulation of the actin cytoskeleton

Graham J. Britton, Rachel Ambler, Danielle J. Clark, Elaine V. Hill, Helen M. Tunbridge, Kerrie E. McNally, Bronwen R. Burton, Philomena Butterweck, Catherine Sabatos-Peyton, Lea A. Hampton-O’neil, Paul Verkade, Christoph Wuelfing, David Cameron Wraith

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

18 Scopus citations

Abstract

Notch is a critical regulator of T cell differentiation and is activated through proteolytic cleavage in response to ligand engagement. Using murine myelin-reactive CD4 T cells, we demonstrate that proximal T cell signaling modulates Notch activation by a spatiotemporally constrained mechanism. The protein kinase PKCθ is a critical mediator of signaling by the T cell antigen receptor and the principal costimulatory receptor CD28. PKCθ selectively inactivates the negative regulator of F-actin generation, Coronin 1A, at the center of the T cell interface with the antigen presenting cell (APC). This allows for effective generation of the large actin-based lamellum required for recruitment of the Notch-processing membrane metalloproteinase ADAM10. Such enhancement of Notch activation is critical for efficient T cell proliferation and Th17 differentiation. We reveal a novel mechanism that, through modulation of the cytoskeleton, controls Notch activation at the T cell:APC interface thereby linking T cell receptor and Notch signaling pathways.

Original language	English
Article number	e20003
Journal	eLife
Volume	6
DOIs	https://doi.org/10.7554/eLife.20003
State	Published - 31 Jan 2017
Externally published	Yes

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Britton, G. J., Ambler, R., Clark, D. J., Hill, E. V., Tunbridge, H. M., McNally, K. E., Burton, B. R., Butterweck, P., Sabatos-Peyton, C., Hampton-O’neil, L. A., Verkade, P., Wuelfing, C., & Wraith, D. C. (2017). PKCθ links proximal T cell and notch signaling through localized regulation of the actin cytoskeleton. eLife, 6, Article e20003. https://doi.org/10.7554/eLife.20003

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title = "PKCθ links proximal T cell and notch signaling through localized regulation of the actin cytoskeleton",

abstract = "Notch is a critical regulator of T cell differentiation and is activated through proteolytic cleavage in response to ligand engagement. Using murine myelin-reactive CD4 T cells, we demonstrate that proximal T cell signaling modulates Notch activation by a spatiotemporally constrained mechanism. The protein kinase PKCθ is a critical mediator of signaling by the T cell antigen receptor and the principal costimulatory receptor CD28. PKCθ selectively inactivates the negative regulator of F-actin generation, Coronin 1A, at the center of the T cell interface with the antigen presenting cell (APC). This allows for effective generation of the large actin-based lamellum required for recruitment of the Notch-processing membrane metalloproteinase ADAM10. Such enhancement of Notch activation is critical for efficient T cell proliferation and Th17 differentiation. We reveal a novel mechanism that, through modulation of the cytoskeleton, controls Notch activation at the T cell:APC interface thereby linking T cell receptor and Notch signaling pathways.",

author = "Britton, \{Graham J.\} and Rachel Ambler and Clark, \{Danielle J.\} and Hill, \{Elaine V.\} and Tunbridge, \{Helen M.\} and McNally, \{Kerrie E.\} and Burton, \{Bronwen R.\} and Philomena Butterweck and Catherine Sabatos-Peyton and Hampton-O{\textquoteright}neil, \{Lea A.\} and Paul Verkade and Christoph Wuelfing and Wraith, \{David Cameron\}",

note = "Publisher Copyright: {\textcopyright} Britton et al.",

year = "2017",

month = jan,

day = "31",

doi = "10.7554/eLife.20003",

language = "English",

volume = "6",

journal = "eLife",

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T1 - PKCθ links proximal T cell and notch signaling through localized regulation of the actin cytoskeleton

AU - Britton, Graham J.

AU - Ambler, Rachel

AU - Clark, Danielle J.

AU - Hill, Elaine V.

AU - Tunbridge, Helen M.

AU - McNally, Kerrie E.

AU - Burton, Bronwen R.

AU - Butterweck, Philomena

AU - Sabatos-Peyton, Catherine

AU - Hampton-O’neil, Lea A.

AU - Verkade, Paul

AU - Wuelfing, Christoph

AU - Wraith, David Cameron

PY - 2017/1/31

Y1 - 2017/1/31

N2 - Notch is a critical regulator of T cell differentiation and is activated through proteolytic cleavage in response to ligand engagement. Using murine myelin-reactive CD4 T cells, we demonstrate that proximal T cell signaling modulates Notch activation by a spatiotemporally constrained mechanism. The protein kinase PKCθ is a critical mediator of signaling by the T cell antigen receptor and the principal costimulatory receptor CD28. PKCθ selectively inactivates the negative regulator of F-actin generation, Coronin 1A, at the center of the T cell interface with the antigen presenting cell (APC). This allows for effective generation of the large actin-based lamellum required for recruitment of the Notch-processing membrane metalloproteinase ADAM10. Such enhancement of Notch activation is critical for efficient T cell proliferation and Th17 differentiation. We reveal a novel mechanism that, through modulation of the cytoskeleton, controls Notch activation at the T cell:APC interface thereby linking T cell receptor and Notch signaling pathways.

AB - Notch is a critical regulator of T cell differentiation and is activated through proteolytic cleavage in response to ligand engagement. Using murine myelin-reactive CD4 T cells, we demonstrate that proximal T cell signaling modulates Notch activation by a spatiotemporally constrained mechanism. The protein kinase PKCθ is a critical mediator of signaling by the T cell antigen receptor and the principal costimulatory receptor CD28. PKCθ selectively inactivates the negative regulator of F-actin generation, Coronin 1A, at the center of the T cell interface with the antigen presenting cell (APC). This allows for effective generation of the large actin-based lamellum required for recruitment of the Notch-processing membrane metalloproteinase ADAM10. Such enhancement of Notch activation is critical for efficient T cell proliferation and Th17 differentiation. We reveal a novel mechanism that, through modulation of the cytoskeleton, controls Notch activation at the T cell:APC interface thereby linking T cell receptor and Notch signaling pathways.

UR - https://www.scopus.com/pages/publications/85013191577

U2 - 10.7554/eLife.20003

DO - 10.7554/eLife.20003

M3 - Article

C2 - 28112644

AN - SCOPUS:85013191577

SN - 2050-084X

VL - 6

JO - eLife

JF - eLife

M1 - e20003

ER -

PKCθ links proximal T cell and notch signaling through localized regulation of the actin cytoskeleton

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