EOMES and IL-10 regulate anti-tumor activity of PD-1<sup>+</sup>CD4<sup>+</sup>T-cells in B-cell Non-Hodgkin lymphoma

Roessner, Philipp M.; Ll, Cid; Lupar, Ekaterina; Roider, Tobias; Bordas, Marie; Schifflers, Christoph; Gaupel, Ann-Christin; Kilpert, Fabian; Krötschel, Marit; Sj, Arnold; Sellner, Leopold; Stilgenbauer, Stephan; Dietrich, Sascha; Lichter, Peter; Ízcue, Ana; Seiffert, Martina

doi:10.1101/2020.03.09.983098

Cited by 5 publications

(9 citation statements)

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“…Of note, increased levels of EOMES-expressing T cells in both effector and memory subsets of TCL1 AT mice, in contrast to non-leukemic control mice were detected (Fig. 2D, E), which confirms previously published data [20,28]. We subsequently assessed EOMES expression levels together with the exhaustion markers PD-1, LAG3, TGIT, and CD244.…”

Section: Eomes + Cd8 + T Cells Accumulate In the Eµ-tcl1 Mouse Model supporting

confidence: 89%

“…The importance of EOMES in adaptive immune control of tumors is further exemplified by a subset of CD4 + T cells that expresses EOMES and shows cytotoxic activity [43]. In line with this, we have recently identified an EOMES + CD4 + T-cell subset, which is increased in CLL and coexpresses PD-1 and LAG3 [28]. Similarly, as observed for CD8 + T cells, EOMES deficiency in CD4 + T cells resulted in faster CLL progression in TCL1 AT mice.…”

Section: Discussionmentioning

confidence: 53%

“…To verify that these observed effects were intrinsic to CD8 + T cells and not induced by other Eomes-deficient cells in Eomes −/− BM chimera, such as previously described for CD4 + T cells [28], we transferred Eomes −/− or WT CD8 + T cells in Rag2 −/− mice and injected these mice 1 day later with Eµ-TCL1 leukemic cells. Similar to the results in the BM chimeric mice, leukemia development was significantly enhanced in mice that received Eomes-deficient CD8 + T cells compared to mice with WT T cells, with higher absolute numbers of CLL cells present in the blood, as well as an increased spleen weight and tumor content in this organ (Fig.…”

Section: Lack Of Eomes In Cd8 + T Cells Leads To Their Impaired Expanmentioning

confidence: 94%

“…To analyze the role of EOMES in T-cell-mediated control of CLL, we generated Eomes −/− BM chimeric mice, as previously described [20,28]. Interestingly, mice with an Eomesdeficient hematopoietic system showed a higher tumor burden compared to Eomes WT chimeric mice at the experimental endpoint, 4 weeks after TCL1 AT.…”

Section: Lack Of Eomes In Cd8 + T Cells Leads To Their Impaired Expanmentioning

confidence: 99%

“…Analyzed mice were males and females of 47-49 weeks of age. The TCL1 AT mouse model has been previously described [28]. Briefly, 2-3 months old C57BL/ 6 female mice were i.v.…”

Section: Tumor Models and Adoptive T-cell Transfer Experimentsmentioning

confidence: 99%

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EOMES is essential for antitumor activity of CD8+ T cells in chronic lymphocytic leukemia

et al. 2021

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Genome-wide association studies identified a single-nucleotide polymorphism (SNP) affecting the transcription factor Eomesodermin (EOMES) associated with a significantly increased risk to develop chronic lymphocytic leukemia (CLL). Epigenetic analyses, RNA sequencing, and flow cytometry revealed that EOMES is not expressed in CLL cells, but in CD8+ T cells for which EOMES is a known master regulator. We thus hypothesized that the increased CLL risk associated with the EOMES SNP might be explained by its negative impact on CD8+ T-cell-mediated immune control of CLL. Flow cytometry analyses revealed a higher EOMES expression in CD8+ T cells of CLL patients compared to healthy individuals, and an accumulation of PD-1+ EOMES+ CD8+ T cells in lymph nodes rather than blood or bone marrow in CLL. This was in line with an observed expansion of EOMES+ CD8+ T cells in the spleen of leukemic Eµ-TCL1 mice. As EOMES expression was highest in CD8+ T cells that express inhibitory receptors, an involvement of EOMES in T-cell exhaustion and dysfunction seems likely. Interestingly, Eomes-deficiency in CD8+ T cells resulted in their impaired expansion associated with decreased CLL control in mice. Overall, these observations suggest that EOMES is essential for CD8+ T-cell expansion and/or maintenance, and therefore involved in adaptive immune control of CLL.

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Section: Eomes + Cd8 + T Cells Accumulate In the Eµ-tcl1 Mouse Model supporting

confidence: 89%

Section: Discussionmentioning

confidence: 53%

Section: Lack Of Eomes In Cd8 + T Cells Leads To Their Impaired Expanmentioning

confidence: 94%

Section: Lack Of Eomes In Cd8 + T Cells Leads To Their Impaired Expanmentioning

confidence: 99%

“…Analyzed mice were males and females of 47-49 weeks of age. The TCL1 AT mouse model has been previously described [28]. Briefly, 2-3 months old C57BL/ 6 female mice were i.v.…”

Section: Tumor Models and Adoptive T-cell Transfer Experimentsmentioning

confidence: 99%

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EOMES is essential for antitumor activity of CD8+ T cells in chronic lymphocytic leukemia

et al. 2021

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T-cells in chronic lymphocytic leukemia: Guardians or drivers of disease?

Roessner

Seiffert

2020

Leukemia

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SummaryChronic lymphocytic leukemia (CLL) is a B-cell malignancy, which is associated with profound alterations and defects in the immune system and a prevalent dependency on the microenvironmental niche. An abnormal T-cell compartment in the blood of CLL patients was already reported 40 years ago. Since then, our knowledge of T-cell characteristics in CLL has grown steadily, but the question of whether T-cells act as pro-tumoral bystander cells or possess anti-tumoral activity is still under debate. Increased numbers of CD4+ T-helper cell subsets are present in the blood of CLL patients, and T-helper cell cytokines have been shown to stimulate CLL cell survival and proliferation in vitro. In line with this, survival and growth of CLL cells in murine xenograft models have been shown to rely on activated CD4+ T-cells. This led to the hypothesis that T-cells are tumor-supportive in CLL. In recent years, evidence for an enrichment of antigen-experienced CD8+ T-cells in CLL has accumulated, and these cells have been shown to control leukemia in a CLL mouse model. Based on this, it was suggested that CD8+ T-cells recognize CLL-specific antigens and exert an anti-leukemia function. As described for other cancer entities, T-cells in CLL express multiple inhibitory receptors, such as PD-1, and lose their functional capacity, leading to an exhaustion phenotype which has been shown to be more severe in T-cells from secondary lymphoid organs compared with peripheral blood. This exhausted phenotype has been suggested to be causative for the poor response of CLL patients to CAR T-cell therapies. In addition, T-cells have been shown to be affected by drugs that are used to treat CLL, which likely impacts therapy response. This review provides an overview of the current knowledge about alterations of T-cells in CLL, including their distribution, function, and exhaustion state in blood and lymphoid organs, and touches also on the topic of how CLL drugs impact on the T-cell compartment and recent results of T-cell-based immunotherapy. We will discuss potential pathological roles of T-cell subsets in CLL and address the question of whether they foster progression or control of disease.

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T-cell dysfunction in chronic lymphocytic leukemia from an epigenetic perspective

Peters

Strefford

Eldering³

et al. 2021

haematol

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Cellular immunotherapeutic approaches such as chimeric antigen receptor (CAR) T-cell therapy in chronic lymphocytic leukemia (CLL) thus far have not met the high expectations. Therefore it is essential to better understand the molecular mechanisms of CLLinduced T-cell dysfunction. Even though a significant number of studies are available on T-cell function and dysfunction in CLL patients, none examine dysfunction at the epigenomic level. In non-malignant T-cell research, epigenomics is widely employed to define the differentiation pathway into T-cell exhaustion. Additionally, metabolic restrictions in the tumor microenvironment that cause T-cell dysfunction are often mediated by epigenetic changes. With this review paper we argue that understanding the epigenetic (dys)regulation in T cells of CLL patients should be leveled to the knowledge we currently have of the neoplastic B cells themselves. This will permit a complete understanding of how these immune cell interactions regulate T- and B-cell function. Here we relate the cellular and phenotypic characteristics of CLL-induced T-cell dysfunction to epigenetic studies of T-cell regulation emerging from chronic viral infection and tumor models. This paper proposes a framework for future studies into the epigenetic regulation of CLL-induced Tcell dysfunction, knowledge that will help to guide improvements in the utility of autologous T-cell based therapies in CLL.

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EOMES and IL-10 regulate anti-tumor activity of PD-1⁺CD4⁺T-cells in B-cell Non-Hodgkin lymphoma

Cited by 5 publications

References 62 publications

EOMES is essential for antitumor activity of CD8+ T cells in chronic lymphocytic leukemia

EOMES is essential for antitumor activity of CD8+ T cells in chronic lymphocytic leukemia

T-cells in chronic lymphocytic leukemia: Guardians or drivers of disease?

T-cell dysfunction in chronic lymphocytic leukemia from an epigenetic perspective

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EOMES and IL-10 regulate anti-tumor activity of PD-1+CD4+T-cells in B-cell Non-Hodgkin lymphoma

Cited by 5 publications

References 62 publications

EOMES is essential for antitumor activity of CD8+ T cells in chronic lymphocytic leukemia

EOMES is essential for antitumor activity of CD8+ T cells in chronic lymphocytic leukemia

T-cells in chronic lymphocytic leukemia: Guardians or drivers of disease?

T-cell dysfunction in chronic lymphocytic leukemia from an epigenetic perspective

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Product

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EOMES and IL-10 regulate anti-tumor activity of PD-1⁺CD4⁺T-cells in B-cell Non-Hodgkin lymphoma