THEMIS: Two Models, Different Thresholds

Choi, Seeyoung; Cornall, Richard J.; Lesourne, Renaud; Love, Paul E.

doi:10.1016/j.it.2017.06.006

Cited by 24 publications

(25 citation statements)

References 62 publications

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“…Interestingly, all eleven genes correlated with low self-reactivity, particularly at the early DP stage of development. This included Themis (Figure 6-figure supplement 2b), which encodes a protein required for modulating TCR signaling during positive selection (Lesourne et al 2009;Patrick et al 2009;Kakugawa et al 2009;Fu et al 2009;Johnson et al 2009;Choi, Warzecha, et al 2017;Choi, Cornall, et al 2017;Mehta et al 2018). Moreover, expression of the curated set of ion channel genes in the ImmGen microarray data set revealed that group 2 genes, whose expression correlated with low self-reactivity, also displayed higher expression in preselection wildtype thymocytes (Figure 6-figure supplement 2c).…”

Section: Resultsmentioning

confidence: 99%

“…A number of molecules have been identified which are involved in modulating TCR signaling in DP thymocytes, and which are downregulated during positive selection. These include the microRNA miR-181a: which enhances TCR signaling by downregulating a set of protein phosphatases (Li et al 2007), Tespa1: a protein that enhances calcium release from the ER (Lyu et al 2019;Liang et al 2017), components of a voltage gated sodium channel (VGSC): that prolongs calcium flux via an unknown mechanism (Lo, Donermeyer, and Allen 2012), and Themis: a TCR associated protein with controversial function (Kakugawa et al 2009;Patrick et al 2009;Lesourne et al 2009;Johnson et al 2009;Fu et al 2009;Choi, Cornall, et al 2017;Fu et al 2013;Choi, Warzecha, et al 2017;Mehta et al 2018). While a diverse set of potential players have been identified, a clear understanding of the mechanisms that render preselection DP thymocytes sensitive to low affinity self-ligands remains elusive.…”

Section: Introductionmentioning

confidence: 99%

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T cell self-reactivity during thymic development dictates the timing of positive selection

Lutes

Steier

McIntyre

et al. 2021

eLife

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Functional tuning of T cells based on their degree of self-reactivity is established during positive selection in the thymus, although how positive selection differs for thymocytes with relatively low versus high self-reactivity is unclear. In addition, preselection thymocytes are highly sensitive to low-affinity ligands, but the mechanism underlying their enhanced TCR sensitivity is not fully understood. Here we show that murine thymocytes with low self-reactivity experience briefer TCR signals and complete positive selection more slowly than those with high self-reactivity. Additionally, we provide evidence that cells with low self-reactivity retain a preselection gene expression signature as they mature, including genes previously implicated in modulating TCR sensitivity and a novel group of ion channel genes. Our results imply that thymocytes with low self-reactivity down-regulate TCR sensitivity more slowly during positive selection, and associate membrane ion channel expression with thymocyte self-reactivity and progress through positive selection.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

T cell self-reactivity during thymic development dictates the timing of positive selection

Lutes

Steier

McIntyre

et al. 2021

eLife

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“…Modulation of SHP-1 activity has been proposed to be the key mechanism of action of Themis, a modulator of TCR signal strength predominantly expressed in DP thymocytes [ 19 , 20 ]. However, it remains controversial whether Themis inhibits or promotes SHP-1 activity [ 19 , 21 ]. Taken together, in thymocytes, the TCR converts signals elicited by pMHC ligands with a continuum of affinities to a digital outcome of positive selection or clonal deletion.…”

Section: Introductionmentioning

confidence: 99%

MicroRNA miR-181—A Rheostat for TCR Signaling in Thymic Selection and Peripheral T-Cell Function

Grewers¹,

Krueger²

2020

IJMS

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The selection of T cells during intra-thymic d evelopment is crucial to obtain a functional and simultaneously not self-reactive peripheral T cell repertoire. However, selection is a complex process dependent on T cell receptor (TCR) thresholds that remain incompletely understood. In peripheral T cells, activation, clonal expansion, and contraction of the active T cell pool, as well as other processes depend on TCR signal strength. Members of the microRNA (miRNA) miR-181 family have been shown to be dynamically regulated during T cell development as well as dependent on the activation stage of T cells. Indeed, it has been shown that expression of miR-181a leads to the downregulation of multiple phosphatases, implicating miR-181a as ‘‘rheostat’’ of TCR signaling. Consistently, genetic models have revealed an essential role of miR-181a/b-1 for the generation of unconventional T cells as well as a function in tuning TCR sensitivity in peripheral T cells during aging. Here, we review these broad roles of miR-181 family members in T cell function via modulating TCR signal strength.

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“…This differential is thought to enable positive selection from low affinity/avidity interactions, prevent the same contacts from activating mature ab T cells, and provide a "safety net" for negative selection to more effectively suppress autoimmunity (6)(7)(8)(9). Although the T lineage-specific Themis protein contributes to this differential in TCR sensitivity between immature and mature ab T cells (9,15,16), the precise mechanisms by which this protein and possibly additional factors "tune" TCR signaling and control ab TCR selection remain to be elucidated.…”

Section: Introductionmentioning

confidence: 99%

The RAG1 Ubiquitin Ligase Domain Enhances the Assembly and Selection of T Cell Receptor Genes to Restrain the Autoimmune Hazard of Generating T Cell Receptor Diversity

Burn

Miot

Gordon

et al. 2021

Preprint

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RAG1/RAG2 (RAG) endonuclease-mediated assembly of diverse lymphocyte antigen receptor genes by V(D)J recombination is critical for the development and immune function of T and B cells. However, this process creates highly self-reactive cells that must be negatively selected to suppress autoimmunity. The RAG1 protein contains a ubiquitin ligase domain that stabilizes RAG1 and stimulates RAG endonuclease activity. We report here that mice lacking RAG1 ubiquitin ligase activity exhibit diminished recombination of T cell receptor (TCR) b and a loci, and impaired thymocyte developmental transitions that require the assembly of these genes and signaling by their proteins. The mice also have reduced expression of TCR signaling proteins within thymocytes, less efficient negative selection of highly self-reactive thymocytes, and mature ab T cells of elevated autoimmune potential. Thus, we propose that the RAG1 ubiquitin ligase domain provides ab T cell developmental stage-specific means to augment TCR signaling and thereby enhance selection for beneficial TCR genes and against ab TCRs possessing high autoimmune potential.

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THEMIS: Two Models, Different Thresholds

Cited by 24 publications

References 62 publications

T cell self-reactivity during thymic development dictates the timing of positive selection

T cell self-reactivity during thymic development dictates the timing of positive selection

MicroRNA miR-181—A Rheostat for TCR Signaling in Thymic Selection and Peripheral T-Cell Function

The RAG1 Ubiquitin Ligase Domain Enhances the Assembly and Selection of T Cell Receptor Genes to Restrain the Autoimmune Hazard of Generating T Cell Receptor Diversity

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