CTLA-4 controls follicular helper T-cell differentiation by regulating the strength of CD28 engagement

Wang, Chun Jing; Heuts, Frank; Ovcinnikovs, Vitalijs; Wardzinski, Lukasz; Bowers, Chantelle E.; Schmidt, Emily M.; Kogimtzis, Alexandros; Kenefeck, Rupert; Sansom, David M.; Walker, Lucy S. K.

doi:10.1073/pnas.1414576112

Cited by 152 publications

(150 citation statements)

References 66 publications

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“…Despite down-regulation of some eTreg-associated genes, CD25 − Tfr cells maintained their expression of the majority of suppressive molecules, most critically CTLA-4, which we and others have demonstrated to have a key role in Tfr-dependent control of Tfh function (41)(42)(43). Notably many of the genes down-regulated in CD25 − Tfr cells, such as Klrg1, Itgae (CD103), Prdm1 (BLIMP-1), Il10, and Gzmb (Granzyme B), are IL-2-dependent (34).…”

Section: Discussionmentioning

confidence: 71%

A distinct subpopulation of CD25⁻T-follicular regulatory cells localizes in the germinal centers

Wing

Kitagawa

Locci

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

165

232

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T-follicular helper (Tfh) cells differentiate through a multistep process, culminating in germinal center (GC) localized GC-Tfh cells that provide support to GC-B cells. T-follicular regulatory (Tfr) cells have critical roles in the control of Tfh cells and GC formation. Although Tfh-cell differentiation is inhibited by IL-2, regulatory T (Treg) cell differentiation and survival depend on it. Here, we describe a CD25− subpopulation within both murine and human PD1+CXCR5+Foxp3+ Tfr cells. It is preferentially located in the GC and can be clearly differentiated from CD25+ non–GC-Tfr, Tfh, and effector Treg (eTreg) cells by the expression of a wide range of molecules. In comparison to CD25+ Tfr and eTreg cells, CD25− Tfr cells partially down-regulate IL-2–dependent canonical Treg features, but retain suppressive function, while simultaneously up-regulating genes associated with Tfh and GC-Tfh cells. We suggest that, similar to Tfh cells, Tfr cells follow a differentiation pathway generating a mature GC-localized subpopulation, CD25− Tfr cells.

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Section: Discussionmentioning

confidence: 71%

A distinct subpopulation of CD25⁻T-follicular regulatory cells localizes in the germinal centers

Wing

Kitagawa

Locci

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

165

232

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“…Indeed, recent studies reported that CTLA-4 controls B cell responses by intrinsic and extrinsic mechanisms (36)(37)(38), in particular at the T follicular helper cell level, a specialized subset of memory lymphocytes (39)(40)(41). Although SRBC challenge is considered as a Tdependent primary humoral response model in rodents, baboons (but also other Old World primates, apes, and humans) are naturally immunized against anti-Gal carbohydrate residues (26) expressed by microorganisms and also other mammals (e.g., sheep).…”

Section: Discussionmentioning

confidence: 99%

Selective CD28 Antagonist Blunts Memory Immune Responses and Promotes Long-Term Control of Skin Inflammation in Nonhuman Primates

Poirier

Chevalier

Mary

et al. 2016

The Journal of Immunology

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Novel therapies that specifically target activation and expansion of pathogenic immune cell subsets responsible for autoimmune attacks are needed to confer long-term remission. Pathogenic cells in autoimmunity include memory T lymphocytes that are long-lived and present rapid recall effector functions with reduced activation requirements. Whereas the CD28 costimulation pathway predominantly controls priming of naive T cells and hence generation of adaptive memory cells, the roles of CD28 costimulation on established memory T lymphocytes and the recall of memory responses remain controversial. In contrast to CD80/86 antagonists (CTLA4-Ig), selective CD28 antagonists blunt T cell costimulation while sparing CTLA-4 and PD-L1–dependent coinhibitory signals. Using a new selective CD28 antagonist, we showed that Ag-specific reactivation of human memory T lymphocytes was prevented. Selective CD28 blockade controlled both cellular and humoral memory recall in nonhuman primates and induced long-term Ag-specific unresponsiveness in a memory T cell–mediated inflammatory skin model. No modification of memory T lymphocytes subsets or numbers was observed in the periphery, and importantly no significant reactivation of quiescent viruses was noticed. These findings indicate that pathogenic memory T cell responses are controlled by both CD28 and CTLA-4/PD-L1 cosignals in vivo and that selectively targeting CD28 would help to promote remission of autoimmune diseases and control chronic inflammation.

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“…Several studies have implicated persistent antigen presentation in Tfh differentiation [117,143], a notion that might fit with the inability of self-antigens to be cleared in autoimmune settings. Interestingly, Tfh differentiation is subject to regulation by a number of pathways that are linked genetically to autoimmunity, including the CD28/cytotoxic T lymphocyte antigen (CTLA)-4 axis [144][145][146][147][148][149][150], IL-2 [127][128][129][130] and the lymphoid-specific tyrosine phosphatase (LYP) encoded by protein tyrosine phosphatase, non-receptor type 22 (PTPN22) [151]. The link between these loci and disease initiation is complex, but modulation of Tfh differentiation adds an additional consideration to the other known roles of the candidate genes in these locations.…”

Section: Il-2 Signalling Impairs Tfh Differentiationmentioning

confidence: 99%

CD4 T cell differentiation in type 1 diabetes

Walker

Herrath

2015

Clinical and Experimental Immunology

146

108

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SummarySusceptibility to type 1 diabetes is associated strongly with human leucocyte antigen (HLA) genes, implicating T cells in disease pathogenesis. In humans, CD8 T cells predominantly infiltrate the islets, yet their activation and propagation probably requires CD4 T cell help. CD4 T cells can select from several differentiation fates following activation, and this choice has profound consequences for their subsequent cytokine production and migratory potential. In turn, these features dictate which other immune cell types T cells interact with and influence, thereby determining downstream effector functions. Obtaining an accurate picture of the type of CD4 T cell differentiation associated with a particular immune-mediated disease therefore constitutes an important clue when planning intervention strategies. Early models of T cell differentiation focused on the dichotomy between T helper type 1 (Th1) and Th2 responses, with type 1 diabetes (T1D) being viewed mainly as a Th1-mediated pathology. However, several additional fate choices have emerged in recent years, including Th17 cells and follicular helper T cells. Here we revisit the issue of T cell differentiation in autoimmune diabetes, highlighting new evidence from both mouse models and patient samples. We assess the strengths and the weaknesses of the Th1 paradigm, review the data on interleukin (IL)-17 production in type 1 diabetes and discuss emerging evidence for the roles of IL-21 and follicular helper T cells in this disease setting. A better understanding of the phenotype of CD4 T cells in T1D will undoubtedly inform biomarker development, improve patient stratification and potentially reveal new targets for therapeutic intervention.

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CTLA-4 controls follicular helper T-cell differentiation by regulating the strength of CD28 engagement

Cited by 152 publications

References 66 publications

A distinct subpopulation of CD25⁻T-follicular regulatory cells localizes in the germinal centers

A distinct subpopulation of CD25⁻T-follicular regulatory cells localizes in the germinal centers

Selective CD28 Antagonist Blunts Memory Immune Responses and Promotes Long-Term Control of Skin Inflammation in Nonhuman Primates

CD4 T cell differentiation in type 1 diabetes

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CTLA-4 controls follicular helper T-cell differentiation by regulating the strength of CD28 engagement

Cited by 152 publications

References 66 publications

A distinct subpopulation of CD25−T-follicular regulatory cells localizes in the germinal centers

A distinct subpopulation of CD25−T-follicular regulatory cells localizes in the germinal centers

Selective CD28 Antagonist Blunts Memory Immune Responses and Promotes Long-Term Control of Skin Inflammation in Nonhuman Primates

CD4 T cell differentiation in type 1 diabetes

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A distinct subpopulation of CD25⁻T-follicular regulatory cells localizes in the germinal centers

A distinct subpopulation of CD25⁻T-follicular regulatory cells localizes in the germinal centers