Donor double‐negative Treg promote allogeneic mixed chimerism and tolerance

He, Kathy M.; Ma, Yuexia; Wang, Shuang; Min, Wei‐Ping; Zhong, Robert; Jevnikar, Anthony M.; Zhang, Zhu‐Xu

doi:10.1002/eji.200737408

Cited by 27 publications

(31 citation statements)

References 70 publications

(104 reference statements)

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“…Subsequent studies reported that DN Tregs displayed antigen specific suppressive activity both in vitro and in vivo (51). DN Tregs not only suppress CD8+ T cell responses, but also inhibit CD4+ T cells (57), B cells (58), NK cells (59), and dendritic cells (DC) (60). …”

Section: Tcrαβ+ Cd4-cd8- Double Negative Tregs (Dn Treg)mentioning

confidence: 99%

“…As might be expected, anti-donor IgM and IgG antibody titers were significantly diminished in recipients of adoptively transferred DN Tregs (58). In a model of murine allogenic bone marrow transfer, DN Tregs supported graft survival through suppressing NK cells by perforin and Fas-FasL dependent pathways (59). …”

Section: Tcrαβ+ Cd4-cd8- Double Negative Tregs (Dn Treg)mentioning

confidence: 99%

“…DN Tregs have been shown to enhance the survival of skin (51, 55, 57), pancreatic islet (55, 68), and heart allografts (65, 69, 70) and heart xenografts (58, 71) and hematopoietic stem cell allografts (59, 67) (Table 3). …”

Section: Tcrαβ+ Cd4-cd8- Double Negative Tregs (Dn Treg)mentioning

confidence: 99%

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Advances on Non-CD4 + Foxp3+ T Regulatory Cells

Ligocki

Niederkorn

2015

Transplantation

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The overwhelming body of research on T regulatory cells (Tregs) has focused on CD4+CD25+Foxp3+ T cells. However, recent years have witnessed a resurgence in interest in CD4-CD8+, CD4-CD8- (double negative; DN), and CD4+Foxp3- Tr1 Tregs and their role in controlling autoimmune diseases and in promoting the survival of organ allografts and xenografts. CD8+ and DN Tregs can arise spontaneously (natural Tregs) or can be induced in situ. Both CD8+ and DN Tregs have been shown to enhance the survival of organ allografts and xenografts. Additionally, both can suppress alloimmune responses by contact-dependent mechanisms by either inducing apoptosis or mediating direct cytolysis of effector T cells. CD8+, DN, and Tr1 Tregs can also act in a contact-independent manner by elaborating soluble immunosuppressive factors such TGF-β and IL-10. Applying CD8+, DN, and Tr1 Tregs for enhancing the survival of organ allografts and xenografts is still in its infancy but holds significant potential. Furthermore, there is a need for a more comprehensive understanding of how current immunosuppressive therapies applied to organ transplantations affect the wide array of Treg populations.

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Section: Tcrαβ+ Cd4-cd8- Double Negative Tregs (Dn Treg)mentioning

confidence: 99%

Section: Tcrαβ+ Cd4-cd8- Double Negative Tregs (Dn Treg)mentioning

confidence: 99%

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Advances on Non-CD4 + Foxp3+ T Regulatory Cells

Ligocki

Niederkorn

2015

Transplantation

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“…Indeed, TCR transgenic and non-transgenic DN T cells can also inhibit NK cells (He et al, 2007; Su et al, 2012), B cells (Zhang et al, 2006; Hillhouse et al, 2010; Ford McIntyre et al, 2011), and dendritic cells (Gao et al, 2011). The combination of their distinct phenotypic characteristics and their unique antigen-specific immunoregulatory properties toward multiple cellular targets has prompted investigators to examine the role of DN T cells in various disease models.…”

Section: Introductionmentioning

confidence: 99%

Immunoregulatory CD4-CD8- T cells as a potential therapeutic tool for transplantation, autoimmunity, and cancer

Hillhouse¹,

Delisle²,

Lesage³

2013

Front. Immun.

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A central objective in organ transplantation and the treatment or prevention of autoimmune disease is the achievement of antigen-specific immune tolerance. An additional challenge in bone marrow transplantation for the treatment of hematological malignancies is the prevention of graft-vs-host disease (GVHD) while maintaining graft-vs-tumor activity. Interestingly, CD4-CD8- (double negative, DN) T cells, which exhibit a unique antigen-specific immunoregulatory potential, appear to exhibit all of the properties to respond to these challenges. Herein, we review the therapeutic potential of immunoregulatory DN T cells in various immunopathological settings, including graft tolerance, GVHD, cancer, and autoimmunity.

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“…Indeed, regulatory DN T cells have been shown to promote allograft and xenograft tolerance (12)(13)(14)(15)(16)(17), limit the incidence of graft versus host disease (17)(18)(19)(20), as well as provide resistance to autoimmune diabetes development in different animal models (21)(22)(23). Specifically, autoimmune-prone mice carry fewer DN T cells, and injection of DN T cells has been shown to be sufficient to reduce the incidence of autoimmune diabetes in two distinct TCR transgenic mouse models (21,22).…”

mentioning

confidence: 99%

The Mouse Idd2 Locus Is Linked to the Proportion of Immunoregulatory Double-Negative T Cells, a Trait Associated with Autoimmune Diabetes Resistance

Collin

Dugas

Pelletier

et al. 2014

The Journal of Immunology

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Autoimmune diseases result from a break in immune tolerance. Various mechanisms of peripheral tolerance can protect against autoimmunity, including immunoregulatory CD4−CD8− double-negative (DN) T cells. Indeed, we have previously shown that diabetes-prone mouse strains exhibit a low proportion of DN T cells relative to that of diabetes-resistant mice, and that a single autologous transfer of DN T cells can impede autoimmune diabetes development, at least in the 3A9 TCR transgenic setting. In this study, we aim to understand the genetic basis for the difference in DN T cell proportion between diabetes-resistant and diabetes-prone mice. We thus perform an unbiased linkage analysis in 3A9 TCR F2 (NOD.H2k × B10.BR) mice and reveal that a locus on chromosome 9, which coincides with Idd2, is linked to the proportion of DN T cells in the lymph nodes. We generate two NOD.H2k.B10-Chr9 congenic mouse strains and validate the role of this genetic interval in defining the proportion of DN T cells. Moreover, we find that the increased proportion of DN T cells in lymphoid organs is associated with a decrease in both diabetes incidence and serum IgG Ab levels. Together, the data suggest that Idd2 is linked to DN T cell proportion and that a physiological increase in DN T cell number may be sufficient to confer resistance to autoimmune diabetes. Altogether, these findings could help identify new candidate genes for the development of therapeutic avenues aimed at modulating DN T cell number for the prevention of autoimmune diseases.

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Donor double‐negative Treg promote allogeneic mixed chimerism and tolerance

Cited by 27 publications

References 70 publications

Advances on Non-CD4 + Foxp3+ T Regulatory Cells

Advances on Non-CD4 + Foxp3+ T Regulatory Cells

Immunoregulatory CD4-CD8- T cells as a potential therapeutic tool for transplantation, autoimmunity, and cancer

The Mouse Idd2 Locus Is Linked to the Proportion of Immunoregulatory Double-Negative T Cells, a Trait Associated with Autoimmune Diabetes Resistance

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