FOXP3, a selective marker for a subset of adult T-cell leukaemia/lymphoma

Roncador, Giovanna; Garcia, Joseph F.; Maestre, Lorena; Lucas, Elena; Menárguez, Javier; Ohshima, Kohichi; Nakamura, Shigeo; Banham, Alison H.; Piris, Miguel Á.

doi:10.1038/sj.leu.2403965

Cited by 128 publications

(105 citation statements)

References 22 publications

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“…Support for the latter hypothesis is provided by recent data demonstrating that HTLV-1 infection of CD4 + CD25 -T cells from healthy donors induces a Treg phenotype by up-regulating CD25 protein, FOXP3 mRNA expression and TGF-b secretion in CD4 + cells [30]. While there have been reports of tumoural FOXP3 expression in an in vitro model of cutaneous T cell lymphoma [31], our data from primary lymphomas do not corroborate these findings, but indicate the presence of a high percentage of "natural" Treg in the skin of mycosis fungoides patients [27,29].…”

Section: Foxp3 Expression In Tumour Cellscontrasting

confidence: 88%

“…mAb (such as 236A/E7) that enable detection of the FOXP3 protein at the single cell level in routinely fixed tissue sections [14] have been used to demonstrate that FOXP3 expression in malignant lymphoma cells is restricted to a poor prognosis subpopulation of patients with adult T cell leukaemia/lymphoma (ATLL) [29]. ATLL has a CD4 + CD25 + phenotype and strong immunosuppressive function, yet it is unclear whether the causal infection by human T lymphotropic virus type 1 (HTLV-1) targets Treg or induces the regulatory phenotype.…”

Section: Foxp3 Expression In Tumour Cellsmentioning

confidence: 99%

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FOXP3⁺ regulatory T cells: Current controversies and future perspectives

2006

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Regulatory T cells (Treg) provide protection from autoimmune disease, graft‐versus‐host disease, transplant rejection and overwhelming tissue destruction during infections. Conversely, high Treg numbers enable cancer cells to evade the host immune response. Thus, Treg are seen as an important tool to manipulate the immune response. However, as the immunological community is trying to move this knowledge from mice to humans, contradictory results regarding the number and function of Treg in various diseases are appearing. This problem arises because we cannot clearly define Treg populations on the basis of expression of CD25 and other cell surface markers in humans. This review addresses the utility of the FOXP3 forkhead transcription factor for the identification of Treg populations and summarizes recent data on the expression of FOXP3 in lymphomas. It is crucial to really understand Treg biology before attempting therapies, including (i) the injection of expanded Treg to cure autoimmune disease or prevent graft‐versus‐host disease or (ii) the depletion or inhibition of Treg in cancer therapy. For instance, new data arising from the study of haematological malignancies highlight the additional complexity of systems where malignant cell populations may also be direct Treg targets.

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Section: Foxp3 Expression In Tumour Cellscontrasting

confidence: 88%

Section: Foxp3 Expression In Tumour Cellsmentioning

confidence: 99%

FOXP3⁺ regulatory T cells: Current controversies and future perspectives

2006

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“…ATL/ATLL cells were initially shown to be positive for mature T-cell surface antigens CD3, CD4, and CD25, and negative for CD8 with rare occasions of double negativity or double positivity for CD4 and CD8 (Hattori et al 1981;Hattori et al 1991). Subsequent studies on the nature of ATL/ATLL cells have shown that they are also positive for regulatory T-cell (Treg) markers, such as FoxP3 (Karube et al 2004;Roncador et al 2005) and the CC chemokine receptor 4 (CCR4) (Yoshie et al 2002). Moreover, several secreted (cytokine) and cell surface-associated (receptor) factors serve as important clues for monitoring the activity and prognosis of patients with ATL/ATLL (Yasuda et al 1988;Yamada et al 1996;Mori and Prager 1998).…”

Section: Introductionmentioning

confidence: 99%

Galectin-9 as a Predictive Marker for the Onset of Immune-Related Adverse Effects Associated with Anti-CCR4 MoAb Therapy in Patients with Adult T Cell Leukemia

Mohammed

Chagan-Yasutan

Ashino

et al. 2017

Tohoku J. Exp. Med.

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Adult T-cell leukemia/lymphoma (ATL/ATLL) is one of the most malignant lymphomas with poor prognosis. ATL/ATLL cells express CC chemokine receptor 4, and mogamulizumab (anti-CCR4 monoclonal antibody) exhibits strong cytotoxicity for ATL/ATLL cells. We analyzed plasma samples of 6 patients with ATL/ATLL treated with chemotherapy followed by mogamulizumab therapy (mogatherapy) for changes in the levels of biomarkers in relation to immune-related adverse effects. As treatment is often associated with skin eruptions, we investigated the profiles of inflammatory cytokines, including galectin-9 (Gal-9), which becomes increased in various infectious diseases and allergic patients. Gal-9, soluble interleukin (IL)-2 receptor, tumor necrosis factor-α, and IL-10 levels were increased before chemotherapy, and Gal-9 levels were associated with the sIL-2 receptor, which reflects tumor burden. Inflammatory levels decreased after chemotherapy. After mogatherapy, 5 of 6 patients attained complete remission (CR), whereas 1 patient showed no response (NR) and died. Among 5 patients with CR, the biomarkers remained low during mogatherapy, except for a 3-5-fold increment in Gal-9 (associated with skin eruptions). A skin biopsy showed infiltration by inflammatory cells and Gal-9 synthesis in areas with CD8 cell infiltration. In the patient with NR, increased levels of Gal-9 and the aforementioned biomarkers were noted 3 days after mogatherapy, followed by opportunistic infections resembling immune reconstitution inflammatory syndrome. Therefore, an increased Gal-9 plasma level in ATL/ATLL indicates tumor burden and reflects immune activation by mogatherapy. These findings may indicate that an increase in the Gal-9 level, a novel immune checkpoint molecule, can reflect immune-related adverse effects of various biotherapies.

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“…Recently, several investigators including ourselves have reported that FOXP3, which is a master control gene for the development and function of CD4 1 CD25 1 naturally occurring regulatory T (Treg) cells, [2][3][4] is expressed in the tumor cells from a subset of patients with ATLL. [5][6][7][8][9][10] Furthermore, we and other investigators have reported that ATLL cells from most patients express CCR4, 11,12 and very recently, Hirahara et al reported that virtually all peripheral blood CD4 1 CD25 high Foxp3 1 Treg cells express high levels of CCR4. 13 Collectively, because most ATLL cells express both CD4 and CD25, 1 based on their phenotypic characteristics, these tumors might originate from CD4 1 CD25 1 FOXP3 1 CCR4 1 Treg cells.…”

mentioning

confidence: 99%

Regulatory T‐cell function of adult T‐cell leukemia/lymphoma cells

Yano

Ishida

Inagaki

et al. 2007

Intl Journal of Cancer

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Adult T-cell leukemia/lymphoma (ATLL) patients are highly immunocompromised, but the underlying mechanism responsible for this state remains obscure. Recent studies demonstrated that FOXP3, which is a master control gene of naturally occurring regulatory T (Treg) cells, is expressed in the tumor cells from a subset of patients with ATLL. Since most ATLL cells express both CD4 and CD25, these tumors might originate from CD4

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FOXP3, a selective marker for a subset of adult T-cell leukaemia/lymphoma

Cited by 128 publications

References 22 publications

FOXP3⁺ regulatory T cells: Current controversies and future perspectives

FOXP3⁺ regulatory T cells: Current controversies and future perspectives

Galectin-9 as a Predictive Marker for the Onset of Immune-Related Adverse Effects Associated with Anti-CCR4 MoAb Therapy in Patients with Adult T Cell Leukemia

Regulatory T‐cell function of adult T‐cell leukemia/lymphoma cells

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FOXP3, a selective marker for a subset of adult T-cell leukaemia/lymphoma

Cited by 128 publications

References 22 publications

FOXP3+ regulatory T cells: Current controversies and future perspectives

FOXP3+ regulatory T cells: Current controversies and future perspectives

Galectin-9 as a Predictive Marker for the Onset of Immune-Related Adverse Effects Associated with Anti-CCR4 MoAb Therapy in Patients with Adult T Cell Leukemia

Regulatory T‐cell function of adult T‐cell leukemia/lymphoma cells

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FOXP3⁺ regulatory T cells: Current controversies and future perspectives

FOXP3⁺ regulatory T cells: Current controversies and future perspectives