Evidence for a Selective Migration of Fetus-Specific CD4+CD25bright Regulatory T Cells from the Peripheral Blood to the Decidua in Human Pregnancy

Tilburgs, Tamara; Roelen, Dave L.; Mast, Barbara J. van der; Groot-Swings, Godelieve M. de; Kleijburg, Carin; Scherjon, Sicco A.; Claas, Frans H.J.

doi:10.4049/jimmunol.180.8.5737

Cited by 322 publications

(301 citation statements)

References 29 publications

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“…Interestingly, pregnant women displayed a lower proportion of cells expressing HLA-DR in the 0.5% CD4 + CD25 highest and the CD4 + cell population compared to controls, which is in line with a very recent report (45). We did not observe a decreased proportion of CD4 dim CD25 high cells showing the CD127 low phenotype, indicating that during pregnancy, Foxp3 is stable and still capable of suppressing CD127 expression.…”

Section: Discussionsupporting

confidence: 79%

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Systemic reduction of functionally suppressive CD4dimCD25highFoxp3+ Tregs in human second trimester pregnancy is induced by progesterone and 17β-estradiol

Mjösberg

Svensson

Johansson

et al. 2009

Journal of Reproductive Immunology

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Section: Discussionsupporting

confidence: 79%

“…We report that Tregs in pregnant women display reduced Foxp3 expression, a finding recently acknowledged also by Tilburgs and colleagues (45). Further, Tregs found in pregnant women seem more activated (increased CD45R0 + and reduced CD45RA + frequencies) compared with non-pregnant women.…”

Section: Discussionsupporting

confidence: 58%

Systemic reduction of functionally suppressive CD4dimCD25highFoxp3+ Tregs in human second trimester pregnancy is induced by progesterone and 17β-estradiol

Mjösberg

Svensson

Johansson

et al. 2009

Journal of Reproductive Immunology

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“…Particular attention has been paid recently to the role of regulatory T cells in maternal-fetal tolerance (11,12). Interestingly, CD4 ϩ CD25 ϩ regulatory T cells have been shown to mediate their suppressive activity through gal1 (40).…”

Section: Discussionmentioning

confidence: 99%

“…Various mechanisms to suppress potentially alloreactive placental T cells and tolerize the maternal immune system toward the fetus have been proposed in mice and humans. These include placental expression of Fas and Fas ligand (6,7), T cell starvation through tryptophan depletion by indolamine 2,3-dioxygenase (8), ligation of the inhibitory ligand PD-L1 expressed on T cells in the gravid uterus (9), Th2 cytokine polarization (10), suppression by CD4 ϩ CD25 ϩ regulatory T cells (11,12), and progesterone-induced Th2-type responses (13). A number of redundant immunosuppressive systems exist at the maternal-fetal interface, not very surprisingly in a system so essential for species survival.…”

mentioning

confidence: 99%

T cell apoptosis at the maternal–fetal interface in early human pregnancy, involvement of galectin-1

Kopcow

Rosetti²,

Leung³

et al. 2008

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

100

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The human fetus is not rejected by the maternal immune system despite expressing paternal antigens. Natural killer cells, the major lymphocyte population of the human decidua (dNKs), express genes with immunomodulatory potential. These include galectin-1 (gal1), a lectin with apoptotic activity on activated CD8 ؉ T cells, Th1 and Th17 CD4 ؉ cells. Although many cell types at the maternalfetal interface also produce gal1, its production by dNKs has been used here to study its function in pregnancy. Media conditioned by dNKs containing gal1 induced apoptosis of activated T cells. This effect was blocked by anti-gal1 antibodies. Decidual T (dT) cells but not peripheral T (pT) cells bound gal1 and presented a distinct glycophenotype compatible with sensitivity to gal1. Annexin V staining, TUNEL, and hypodiploidy showed a substantial proportion of apoptotic dT cells. Immunohistochemistry revealed widespread expression of gal1 as well as periglandular apoptotic dT foci that colocalized with dNKs. Thus, secretion of gal1 by dNKs and other decidual cells contributes to the generation of an immuneprivileged environment at the maternal-fetal interface.maternal-fetal tolerance ͉ NK cells ͉ lectin ͉ decidua

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“…Adoptive transfer reconstitution of BALB/c nude mice with lymphocytes depleted of Tregs results in smaller litters from allogenic matings (9). Treg populations peak in peripheral blood lymphocytes during the second trimester of human pregnancies and accumulate in the decidua (10).…”

mentioning

confidence: 99%

Pregnancy induces a fetal antigen-specific maternal T regulatory cell response that contributes to tolerance

Kahn

Baltimore

2010

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

213

202

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A fetus is inherently antigenic to its mother and yet is not rejected. The T regulatory (Treg) subset of CD4 + T cells can limit immune responses and has been implicated in maternal tolerance of the fetus. Using virgin inbred mice undergoing a first syngenic pregnancy, in which only the male fetuses are antigenic, we demonstrate a maternal splenocyte proliferative response to the CD4 + T cell restricted epitope of the male antigen (H-Y) in proportion to the fetal antigen load. A portion of the maternal immune response to fetal antigens is Treg in nature. The bystander suppressive function of pregnancy-generated Tregs requires the presence of the fetal antigen, demonstrating their inherent antigen specificity. In vivo targeting of diphtheria toxin to kill Tregs leads to a lower fraction of live male offspring and a selective reduction in mass of the surviving males. Thus, Tregs generated in the context of pregnancy function in an antigen-specific manner to limit the maternal immune response to the fetus in a successful pregnancy.

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Evidence for a Selective Migration of Fetus-Specific CD4+CD25bright Regulatory T Cells from the Peripheral Blood to the Decidua in Human Pregnancy

Cited by 322 publications

References 29 publications

Systemic reduction of functionally suppressive CD4dimCD25highFoxp3+ Tregs in human second trimester pregnancy is induced by progesterone and 17β-estradiol

Systemic reduction of functionally suppressive CD4dimCD25highFoxp3+ Tregs in human second trimester pregnancy is induced by progesterone and 17β-estradiol

T cell apoptosis at the maternal–fetal interface in early human pregnancy, involvement of galectin-1

Pregnancy induces a fetal antigen-specific maternal T regulatory cell response that contributes to tolerance

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