TCR ITAM multiplicity is required for the generation of follicular helper T-cells

Su Jin Hwang; Amy C. Palin; Li Qi Li; Ki Duk Song; Jan Lee; Jasmin Herz; Noah Tubo; Hamlet Chu; Marion Pepper; Renaud Lesourne; Ekaterina Zvezdova; Julia Pinkhasov; Marc K. Jenkins; Dorian McGavern; Paul E. Love

doi:10.1038/ncomms7982

TCR ITAM multiplicity is required for the generation of follicular helper T-cells

Su Jin Hwang
, Amy C. Palin
, Li Qi Li
, Ki Duk Song
, Jan Lee
, Jasmin Herz
, Noah Tubo
, Hamlet Chu
, Marion Pepper
, Renaud Lesourne
, Ekaterina Zvezdova
, Julia Pinkhasov
, Marc K. Jenkins
, Dorian McGavern
, Paul E. Love^*

^*Corresponding author for this work

Department of Agricultural Convergence Technology

National Institutes of Health
George Washington University
Hankyong National University
University of Minnesota Twin Cities
Sanofi-Aventis
University of California at Berkeley
University of Washington
Institut Toulousain des Maladies Infectieuses et Inflammatoires (Infinity)
Institut national de la santé et de la recherche médicale
CNRS
Université Toulouse III
Columbia University
University of California at Los Angeles

Research output: Contribution to journal › Journal article › peer-review

30 Scopus citations

Abstract

The T-cell antigen receptor (TCR) complex contains 10 copies of a di-tyrosine Immunoreceptor-Tyrosine-based-Activation-Motif (ITAM) that initiates TCR signalling by recruiting protein tyrosine kinases. ITAM multiplicity amplifies TCR signals, but the importance of this capability for T-cell responses remains undefined. Most TCR ITAMs (6 of 10) are contributed by the CD3ζ subunits. We generated 'knock-in' mice that express non-signalling CD3ζ chains in lieu of wild-type CD3ζ. Here we demonstrate that ITAM multiplicity is important for the development of innate-like T-cells and follicular helper T-cells, events that are known to require strong/sustained TCR-ligand interactions, but is not essential for 'general' T-cell responses including proliferation and cytokine production or for the generation of a diverse antigen-reactive TCR repertoire.

Original language	English
Article number	6982
Journal	Nature Communications
Volume	6
DOIs	https://doi.org/10.1038/ncomms7982
State	Published - 2015.05.11

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10.1038/ncomms7982

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@article{c9a85bf789f94f85919e4c1c10d40f6c,

title = "TCR ITAM multiplicity is required for the generation of follicular helper T-cells",

abstract = "The T-cell antigen receptor (TCR) complex contains 10 copies of a di-tyrosine Immunoreceptor-Tyrosine-based-Activation-Motif (ITAM) that initiates TCR signalling by recruiting protein tyrosine kinases. ITAM multiplicity amplifies TCR signals, but the importance of this capability for T-cell responses remains undefined. Most TCR ITAMs (6 of 10) are contributed by the CD3ζ subunits. We generated 'knock-in' mice that express non-signalling CD3ζ chains in lieu of wild-type CD3ζ. Here we demonstrate that ITAM multiplicity is important for the development of innate-like T-cells and follicular helper T-cells, events that are known to require strong/sustained TCR-ligand interactions, but is not essential for 'general' T-cell responses including proliferation and cytokine production or for the generation of a diverse antigen-reactive TCR repertoire.",

author = "Hwang, \{Su Jin\} and Palin, \{Amy C.\} and Li, \{Li Qi\} and Song, \{Ki Duk\} and Jan Lee and Jasmin Herz and Noah Tubo and Hamlet Chu and Marion Pepper and Renaud Lesourne and Ekaterina Zvezdova and Julia Pinkhasov and Jenkins, \{Marc K.\} and Dorian McGavern and Love, \{Paul E.\}",

note = "Publisher Copyright: {\textcopyright} 2015 Macmillan Publishers Limited.",

year = "2015",

month = may,

day = "11",

doi = "10.1038/ncomms7982",

language = "English",

volume = "6",

journal = "Nature Communications",

issn = "2041-1723",

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T1 - TCR ITAM multiplicity is required for the generation of follicular helper T-cells

AU - Hwang, Su Jin

AU - Palin, Amy C.

AU - Li, Li Qi

AU - Song, Ki Duk

AU - Lee, Jan

AU - Herz, Jasmin

AU - Tubo, Noah

AU - Chu, Hamlet

AU - Pepper, Marion

AU - Lesourne, Renaud

AU - Zvezdova, Ekaterina

AU - Pinkhasov, Julia

AU - Jenkins, Marc K.

AU - McGavern, Dorian

AU - Love, Paul E.

PY - 2015/5/11

Y1 - 2015/5/11

N2 - The T-cell antigen receptor (TCR) complex contains 10 copies of a di-tyrosine Immunoreceptor-Tyrosine-based-Activation-Motif (ITAM) that initiates TCR signalling by recruiting protein tyrosine kinases. ITAM multiplicity amplifies TCR signals, but the importance of this capability for T-cell responses remains undefined. Most TCR ITAMs (6 of 10) are contributed by the CD3ζ subunits. We generated 'knock-in' mice that express non-signalling CD3ζ chains in lieu of wild-type CD3ζ. Here we demonstrate that ITAM multiplicity is important for the development of innate-like T-cells and follicular helper T-cells, events that are known to require strong/sustained TCR-ligand interactions, but is not essential for 'general' T-cell responses including proliferation and cytokine production or for the generation of a diverse antigen-reactive TCR repertoire.

AB - The T-cell antigen receptor (TCR) complex contains 10 copies of a di-tyrosine Immunoreceptor-Tyrosine-based-Activation-Motif (ITAM) that initiates TCR signalling by recruiting protein tyrosine kinases. ITAM multiplicity amplifies TCR signals, but the importance of this capability for T-cell responses remains undefined. Most TCR ITAMs (6 of 10) are contributed by the CD3ζ subunits. We generated 'knock-in' mice that express non-signalling CD3ζ chains in lieu of wild-type CD3ζ. Here we demonstrate that ITAM multiplicity is important for the development of innate-like T-cells and follicular helper T-cells, events that are known to require strong/sustained TCR-ligand interactions, but is not essential for 'general' T-cell responses including proliferation and cytokine production or for the generation of a diverse antigen-reactive TCR repertoire.

UR - https://www.scopus.com/pages/publications/84929223491

U2 - 10.1038/ncomms7982

DO - 10.1038/ncomms7982

M3 - Journal article

C2 - 25959494

AN - SCOPUS:84929223491

SN - 2041-1723

VL - 6

JO - Nature Communications

JF - Nature Communications

M1 - 6982

ER -

TCR ITAM multiplicity is required for the generation of follicular helper T-cells

Abstract

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