PreTCR and TCRγδ Signal Initiation in Thymocyte Progenitors Does Not Require Domains Implicated in Receptor Oligomerization

Mahtani-Patching, Juliet; Neves, Joana F.; Pang, Dick John; Stoenchev, Kostadin V.; Aguirre-Blanco, Ana M.; Silva‐Santos, Bruno; Pennington, Daniel J.

doi:10.1126/scisignal.2001765

Cited by 26 publications

(26 citation statements)

References 36 publications

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“…Thymic ligand-independent signalling was similarly proposed for TCRgd, possibly mediated by oligomerisation of the variable region of TCRd [7]. However, a recent study has suggested that TCRgd complexes that lack variable domains, or that lack both variable and constant Ig-like domains, can still initiate signals that drive Recombination activating gene 2 (RAG-2)-deficient thymocytes toward a gd-like fate [6]. This implies that appropriate surface pairing of TCRg and TCRd chains that possibly bring CD3e-containing signalling modules into close proximity of available lymphocyte-specific protein tyrosine kinase (Lck) is sufficient for TCRgd signal initiation in DN thymocytes.…”

Section: Ligand-independent Tcrgd Signallingmentioning

confidence: 94%

“…This implies that appropriate surface pairing of TCRg and TCRd chains that possibly bring CD3e-containing signalling modules into close proximity of available lymphocyte-specific protein tyrosine kinase (Lck) is sufficient for TCRgd signal initiation in DN thymocytes. Thus, strong TCRgd signalling may not only be a consequence of ligand engagement; additionally, efficiently paired TCRg/TCRd chains that are expressed at the cell surface above a certain critical threshold will also commit DN progenitors to a gd cell fate [6].…”

Section: Ligand-independent Tcrgd Signallingmentioning

confidence: 99%

“…Moreover, ligandmediated positive and negative selection through TCRgd remain poorly understood, as too does the correlation between thymic TCRgd signalling and subsequent gd effector fates. Here, we build on recent studies that have assessed the initiation and consequences of TCRgd signalling in immature thymocytes [5][6][7], to propose that thymic TCRgd-ligand engagement versus ligand-independent TCRgd signalling may differentially impose innate-like versus adaptive-like features on developing gd cells.…”

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confidence: 98%

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T cell receptor signalling in γδ cell development: strength isn’t everything

Turchinovich

Pennington

2011

Trends in Immunology

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Section: Ligand-independent Tcrgd Signallingmentioning

confidence: 94%

Section: Ligand-independent Tcrgd Signallingmentioning

confidence: 99%

mentioning

confidence: 98%

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T cell receptor signalling in γδ cell development: strength isn’t everything

Turchinovich

Pennington

2011

Trends in Immunology

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“…Self-oligomerization of γδTCR at the cell surface of precursor thymocytes induces their differentiation into mature γδT cells (12,13). It has been proposed that γδTCR-ligand interaction determines the effector function of γδT cells (14).…”

Section: Introductionmentioning

confidence: 99%

γδTCR recruits the Syk/PI3K axis to drive proinflammatory differentiation program

Muro¹,

Nitta²,

Nakano³

et al. 2017

Journal of Clinical Investigation

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Results Preferential requirement of Syk rather than Zap70 in γδTCR signalsand γδT cell development. To characterize the intracellular signal γδT cells produce inflammatory cytokines and have been implicated in the pathogenesis of cancer, infectious diseases, and autoimmunity. The T cell receptor (TCR) signal transduction that specifically regulates the development of IL-17-producing γδT (γδT17) cells largely remains unclear. Here, we showed that the receptor proximal tyrosine kinase Syk is essential for γδTCR signal transduction and development of γδT17 in the mouse thymus. Zap70, another tyrosine kinase essential for the development of αβT cells, failed to functionally substitute for Syk in the development of γδT17. Syk induced the activation of the PI3K/Akt pathway upon γδTCR stimulation. Mice deficient in PI3K signaling exhibited a complete loss of γδT17, without impaired development of IFN-γ-producing γδT cells. Moreover, γδT17-dependent skin inflammation was ameliorated in mice deficient in RhoH, an adaptor known to recruit Syk. Thus, we deciphered lineage-specific TCR signaling and identified the Syk/PI3K pathway as a critical determinant of proinflammatory γδT cell differentiation.

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“…Notably, TCRgd can also mediate bselection-like differentiation to the DP stage. This is most evident in animals unable to express a functional pre-TCR, in TCRgd Tg mice in vivo (8,10,(19)(20)(21)(22)(23), and in cultures in which TCRgdexpressing progenitor cells are allowed to develop in vitro (24)(25)(26). Like b-selected DP cells, gd-selected DP cells silence TCRg gene expression and undergo TCRa rearrangements, indicating that they are bona fide ab-lineage cells (21).…”

mentioning

confidence: 99%

Temporal Predisposition to αβ and γδ T Cell Fates in the Thymus

Pereira

Boucontet

Cumano

2012

The Journal of Immunology

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How T cell progenitors engage into the γδ or αβ T cell lineages is a matter of intense debate. In this study, we analyzed the differentiation potential of single thymocytes from wild-type and TCRγδ-transgenic mice at two sequential early developmental stages. Double-negative (DN) 3 progenitors from both wild-type and transgenic mice retain the capacity to engage into both pathways, indicating that full commitment is only completed after this stage. More importantly, DN2 and DN3 progenitors from TCRγδ transgenic mice have strong biases for opposite fates, indicating that developmentally regulated changes, other than the production of a functional TCR, altered their likelihood to become a γδ or an αβ T cell. Thus, unlike the differentiation in other hematopoietic lineages, T cell progenitors did not restrict, but rather switch their differentiation potential as they developed.

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PreTCR and TCRγδ Signal Initiation in Thymocyte Progenitors Does Not Require Domains Implicated in Receptor Oligomerization

Cited by 26 publications

References 36 publications

T cell receptor signalling in γδ cell development: strength isn’t everything

T cell receptor signalling in γδ cell development: strength isn’t everything

γδTCR recruits the Syk/PI3K axis to drive proinflammatory differentiation program

Temporal Predisposition to αβ and γδ T Cell Fates in the Thymus

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