Butyrophilin-like 3 Directly Binds a Human Vγ4+ T Cell Receptor Using a Modality Distinct from Clonally-Restricted Antigen

Willcox, Carrie R.; Vantourout, Pierre; Salim, Mahboob; Zlatareva, Iva; Melandri, Daisy; Zanardo, Leonor; George, Roger; Kjær, Svend; Jeeves, Mark; Mohammed, Fiyaz; Hayday, Adrian; Willcox, Benjamin E.

doi:10.1016/j.immuni.2019.09.006

Cited by 117 publications

(171 citation statements)

References 55 publications

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“…In brief, pAgs are metabolic products that interact with the butyrophilin family member BTN3A1 and activate Vγ9Vδ2 T cells in a BTN2A1-dependent manner [15,16,18,21,[50][51][52]. BTN2A1 has been shown to interact with BTN3A1 and binds Vγ9 + chains via germline-encoded residues in the hypervariable region 4 (HV4) and CDR2, similar to BTNL3 interactions with Vγ4 + chains [18,19,21]. According to Rigau and colleagues, phosphoantigen reactivity depends on the Vγ9JP CDR3 loop and CDR2 residues of Vδ2 chains, that seem to form a second interaction site with another molecule (potentially BTN3A1) on the TCR surface [43,45,53].…”

Section: Introductionmentioning

confidence: 99%

“…In particular, EPCR and annexin A2, as well as phosphorylated metabolites of isoprenoid synthesis, were described as serving as self-antigens that indicate cellular stress [5,[11][12][13]. Most importantly, B7 receptor family-like butyrophilin (BTN) and butyrophilin-like (BTNL) molecules have been implied in the development of specific epithelial and circulating γδ T cell subsets [14][15][16][17] and as direct γδ TCRs ligands [18][19][20][21]. Advances in next-generation sequencing (NGS) analysis of human γδ TCR repertoires, together with the recent identification of γδ TCR ligands, shed light on the vast TCR diversity of human γδ T cells, thereby pointing to a complex role in health and disease.…”

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confidence: 99%

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Human γδ TCR Repertoires in Health and Disease

Fichtner

Ravens

Prinz

2020

Cells

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The T cell receptor (TCR) repertoires of γδ T cells are very different to those of αβ T cells. While the theoretical TCR repertoire diversity of γδ T cells is estimated to exceed the diversity of αβ T cells by far, γδ T cells are still understood as more invariant T cells that only use a limited set of γδ TCRs. Most of our current knowledge of human γδ T cell receptor diversity builds on specific monoclonal antibodies that discriminate between the two major subsets, namely Vδ2+ and Vδ1+ T cells. Of those two subsets, Vδ2+ T cells seem to better fit into a role of innate T cells with semi-invariant TCR usage, as compared to an adaptive-like biology of some Vδ1+ subsets. Yet, this distinction into innate-like Vδ2+ and adaptive-like Vδ1+ γδ T cells does not quite recapitulate the full diversity of γδ T cell subsets, ligands and interaction modes. Here, we review how the recent introduction of high-throughput TCR repertoire sequencing has boosted our knowledge of γδ T cell repertoire diversity beyond Vδ2+ and Vδ1+ T cells. We discuss the current understanding of clonal composition and the dynamics of human γδ TCR repertoires in health and disease.

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Section: Introductionmentioning

confidence: 99%

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confidence: 99%

Human γδ TCR Repertoires in Health and Disease

Fichtner

Ravens

Prinz

2020

Cells

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“…S1G). Although it remains to be tested if any of these positively charged amino acids in the framework regions are involved in recognition of the polyanionic ligands, it is interesting to note that germline‐encoded Vγ sequences were recently shown to be involved in recognition of butyrophilin family members by mouse Vγ7 and human Vγ4 TCRs . Results reported here also demonstrate that the amino acid sequences of CDR3 regions impact the strength of spontaneous reactivity.…”

Section: Discussionmentioning

confidence: 62%

Recognition of synthetic polyanionic ligands underlies “spontaneous” reactivity of Vγ1 γδTCRs

Dunst

Glaros

Englmaier

et al. 2020

Journal of Leukocyte Biology

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Although γδTCRs were discovered more than 30 yr ago, principles of antigen recognition by these receptors remain unclear and the nature of these antigens is largely elusive. Numerous studies reported that T cell hybridomas expressing several Vγ1‐containing TCRs, including the Vγ1Vδ6 TCR of γδNKT cells, spontaneously secrete cytokines. This property was interpreted as recognition of a self‐ligand expressed on the hybridoma cells themselves. Here, we revisited this finding using a recently developed reporter system and live single cell imaging. We confirmed strong spontaneous signaling by Vγ1Vδ6 and related TCRs, but not by TCRs from several other γδ or innate‐like αβ T cells, and demonstrated that both γ and δ chains contributed to this reactivity. Unexpectedly, live single cell imaging showed that activation of this signaling did not require any interaction between cells. Further investigation revealed that the signaling is instead activated by interaction with negatively charged surfaces abundantly present under regular cell culture conditions and was abrogated when noncharged cell culture vessels were used. This mode of TCR signaling activation was not restricted to the reporter cell lines, as interaction with negatively charged surfaces also triggered TCR signaling in ex vivo Vγ1 γδ T cells. Taken together, these results explain long‐standing observations on the spontaneous reactivity of Vγ1Vδ6 TCR and demonstrate an unexpected antigen presentation‐independent mode of TCR activation by a spectrum of chemically unrelated polyanionic ligands.

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“…In a first attempt to integrate lessons learned from Skint1‐DETC and Btnl1/6‐Vγ7 + IELs while also taking into account the fact that γδ TCRs are able to recognize Ags in an adaptive manner (see Silva‐Santos and Strid), 161 it was suggested that the γδ TCR can combine 2 features by exhibiting a dual reactivity using spatially distinct regions for agonist selection and Ag responsiveness 162,163 . This specific mode of recognition was termed “adaptate” reflecting the blend of innate and adaptive features that is unique to the γδTCR 164 and could recently be supported by a study showing direct binding of a human Vγ4 + TCR and BTNL3 163 . Further evidences for this interesting concept should be obtainable by carefully choosing transgenic TCR‐γ in combination with TCR‐δ lines and analyzing the γδ T cell development in the presence or absence of the respective Btnl‐members.…”

Section: The Butyrophilin Family—a Major Regulator Of γδ Biologymentioning

confidence: 95%

Resolving the mystery—How TCR transgenic mouse models shed light on the elusive case of gamma delta T cells

Hahn

Winkler

2020

Journal of Leukocyte Biology

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Cutting‐edge questions in αβ T cell biology were addressed by investigating a range of different genetically modified mouse models. In comparison, the γδ T cell field lacks behind on the availability of such models. Nevertheless, transgenic mouse models proved useful for the investigation of γδ T cell biology and their stepwise development in the thymus. In general, animal models and especially mouse models give access to a wide range of opportunities of modulating γδ T cells, which is unachievable in human beings. Because of their complex biology and specific tissue tropism, it is especially challenging to investigate γδ T cells in in vitro experiments since they might not reliably reflect their behavior and phenotype under physiologic conditions. This review aims to provide a comprehensive historical overview about how different transgenic mouse models contributed in regards of the understanding of γδ T cell biology, whereby a special focus is set on studies including the elusive role of the γδTCR. Furthermore, evolutionary and translational remarks are discussed under the aspect of future implications for the field. The ultimate full understanding of γδ T cells will pave the way for their usage as a powerful new tool in immunotherapy.

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Butyrophilin-like 3 Directly Binds a Human Vγ4+ T Cell Receptor Using a Modality Distinct from Clonally-Restricted Antigen

Cited by 117 publications

References 55 publications

Human γδ TCR Repertoires in Health and Disease

Human γδ TCR Repertoires in Health and Disease

Recognition of synthetic polyanionic ligands underlies “spontaneous” reactivity of Vγ1 γδTCRs

Resolving the mystery—How TCR transgenic mouse models shed light on the elusive case of gamma delta T cells

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