Fine-tuning of T-cell development by the CD3γ di-leucine-based TCR-sorting motif

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Fine-tuning of T-cell development by the CD3γ di-leucine-based TCR-sorting motif. / Lauritsen, Jens Peter Holst; Boding, Lasse; Buus, Terkild B; Kongsbak-Wismann, Martin; Levring, Trine B; Rode, Anna Kathrine Obelitz; Bonefeld, Charlotte Menné; Geisler, Carsten.

In: International Immunology, Vol. 27, No. 8, 08.2015, p. 393-404.

Research output: Contribution to journalJournal articleResearchpeer-review

Harvard

Lauritsen, JPH, Boding, L, Buus, TB, Kongsbak-Wismann, M, Levring, TB, Rode, AKO, Bonefeld, CM & Geisler, C 2015, 'Fine-tuning of T-cell development by the CD3γ di-leucine-based TCR-sorting motif', International Immunology, vol. 27, no. 8, pp. 393-404. https://doi.org/10.1093/intimm/dxv022

APA

Lauritsen, J. P. H., Boding, L., Buus, T. B., Kongsbak-Wismann, M., Levring, T. B., Rode, A. K. O., Bonefeld, C. M., & Geisler, C. (2015). Fine-tuning of T-cell development by the CD3γ di-leucine-based TCR-sorting motif. International Immunology, 27(8), 393-404. https://doi.org/10.1093/intimm/dxv022

Vancouver

Lauritsen JPH, Boding L, Buus TB, Kongsbak-Wismann M, Levring TB, Rode AKO et al. Fine-tuning of T-cell development by the CD3γ di-leucine-based TCR-sorting motif. International Immunology. 2015 Aug;27(8):393-404. https://doi.org/10.1093/intimm/dxv022

Author

Lauritsen, Jens Peter Holst ; Boding, Lasse ; Buus, Terkild B ; Kongsbak-Wismann, Martin ; Levring, Trine B ; Rode, Anna Kathrine Obelitz ; Bonefeld, Charlotte Menné ; Geisler, Carsten. / Fine-tuning of T-cell development by the CD3γ di-leucine-based TCR-sorting motif. In: International Immunology. 2015 ; Vol. 27, No. 8. pp. 393-404.

Bibtex

@article{faf9afeed61b48b998239d9375a5fff5,
title = "Fine-tuning of T-cell development by the CD3γ di-leucine-based TCR-sorting motif",
abstract = "The CD3γ di-leucine-based (diL) receptor-sorting motif plays a central role in TCR down-regulation and in clonal expansion of virus-specific T cells. However, the role of the CD3γ diL motif in T-cell development is not known. In this study, we show that protein kinase C-induced TCR down-regulation is abolished in thymocytes from CD3γLLAA mice with a mutated CD3γ diL motif, and that CD3γLLAA mice have reduced numbers of thymocytes compared with aged-matched wild-type mice. We found that early thymocyte development at the β-selection checkpoint is impaired resulting in reduced numbers of double negative (DN) 4 cells in CD3γLLAA mice. This was not caused by reduced proliferation but most probably by increased down-regulation of the antiapoptotic molecule Bcl-2 causing enhanced apoptosis during the transition from the DN3 to the DN4 stage. In contrast, proliferation of immature CD8 single positive (ISP) thymocytes was increased resulting in normal numbers of ISP in CD3γLLAA mice. Despite the normal numbers of ISP, CD3γLLAA mice had reduced numbers of double positive and SP thymocytes indicating that the CD3γ diL motif also affected later stages of T-cell development. In accordance, we found that positive and negative selection, differentiation toward CD4 and CD8 SP T cells and the development of nonconventional T cells were affected in CD3γLLAA mice. In conclusion, our study identifies an important role of the CD3γ diL motif in T-cell development most probably mediated by its fine-tuning of pre-TCR and TCR expression, down-regulation and signaling.",
author = "Lauritsen, {Jens Peter Holst} and Lasse Boding and Buus, {Terkild B} and Martin Kongsbak-Wismann and Levring, {Trine B} and Rode, {Anna Kathrine Obelitz} and Bonefeld, {Charlotte Menn{\'e}} and Carsten Geisler",
note = "{\textcopyright} The Japanese Society for Immunology. 2015. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.",
year = "2015",
month = aug,
doi = "10.1093/intimm/dxv022",
language = "English",
volume = "27",
pages = "393--404",
journal = "International Immunology",
issn = "0953-8178",
publisher = "Oxford University Press",
number = "8",

}

RIS

TY - JOUR

T1 - Fine-tuning of T-cell development by the CD3γ di-leucine-based TCR-sorting motif

AU - Lauritsen, Jens Peter Holst

AU - Boding, Lasse

AU - Buus, Terkild B

AU - Kongsbak-Wismann, Martin

AU - Levring, Trine B

AU - Rode, Anna Kathrine Obelitz

AU - Bonefeld, Charlotte Menné

AU - Geisler, Carsten

N1 - © The Japanese Society for Immunology. 2015. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.

PY - 2015/8

Y1 - 2015/8

N2 - The CD3γ di-leucine-based (diL) receptor-sorting motif plays a central role in TCR down-regulation and in clonal expansion of virus-specific T cells. However, the role of the CD3γ diL motif in T-cell development is not known. In this study, we show that protein kinase C-induced TCR down-regulation is abolished in thymocytes from CD3γLLAA mice with a mutated CD3γ diL motif, and that CD3γLLAA mice have reduced numbers of thymocytes compared with aged-matched wild-type mice. We found that early thymocyte development at the β-selection checkpoint is impaired resulting in reduced numbers of double negative (DN) 4 cells in CD3γLLAA mice. This was not caused by reduced proliferation but most probably by increased down-regulation of the antiapoptotic molecule Bcl-2 causing enhanced apoptosis during the transition from the DN3 to the DN4 stage. In contrast, proliferation of immature CD8 single positive (ISP) thymocytes was increased resulting in normal numbers of ISP in CD3γLLAA mice. Despite the normal numbers of ISP, CD3γLLAA mice had reduced numbers of double positive and SP thymocytes indicating that the CD3γ diL motif also affected later stages of T-cell development. In accordance, we found that positive and negative selection, differentiation toward CD4 and CD8 SP T cells and the development of nonconventional T cells were affected in CD3γLLAA mice. In conclusion, our study identifies an important role of the CD3γ diL motif in T-cell development most probably mediated by its fine-tuning of pre-TCR and TCR expression, down-regulation and signaling.

AB - The CD3γ di-leucine-based (diL) receptor-sorting motif plays a central role in TCR down-regulation and in clonal expansion of virus-specific T cells. However, the role of the CD3γ diL motif in T-cell development is not known. In this study, we show that protein kinase C-induced TCR down-regulation is abolished in thymocytes from CD3γLLAA mice with a mutated CD3γ diL motif, and that CD3γLLAA mice have reduced numbers of thymocytes compared with aged-matched wild-type mice. We found that early thymocyte development at the β-selection checkpoint is impaired resulting in reduced numbers of double negative (DN) 4 cells in CD3γLLAA mice. This was not caused by reduced proliferation but most probably by increased down-regulation of the antiapoptotic molecule Bcl-2 causing enhanced apoptosis during the transition from the DN3 to the DN4 stage. In contrast, proliferation of immature CD8 single positive (ISP) thymocytes was increased resulting in normal numbers of ISP in CD3γLLAA mice. Despite the normal numbers of ISP, CD3γLLAA mice had reduced numbers of double positive and SP thymocytes indicating that the CD3γ diL motif also affected later stages of T-cell development. In accordance, we found that positive and negative selection, differentiation toward CD4 and CD8 SP T cells and the development of nonconventional T cells were affected in CD3γLLAA mice. In conclusion, our study identifies an important role of the CD3γ diL motif in T-cell development most probably mediated by its fine-tuning of pre-TCR and TCR expression, down-regulation and signaling.

U2 - 10.1093/intimm/dxv022

DO - 10.1093/intimm/dxv022

M3 - Journal article

C2 - 25920998

VL - 27

SP - 393

EP - 404

JO - International Immunology

JF - International Immunology

SN - 0953-8178

IS - 8

ER -

ID: 158578366