Crosstalk between decidual NK and CD14
            <sup>+</sup>
            myelomonocytic cells results in induction of Tregs and immunosuppression

Vacca, Paola; Cantoni, Claudia; Vitale, Massimo; Prato, Carola; Canegallo, Francesca; Fenoglio, Daniela; Ragni, Nicola; Moretta, Alessandro; Mingari, Maria Cristina

doi:10.1073/pnas.1001749107

Cited by 213 publications

(192 citation statements)

References 56 publications

(84 reference statements)

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“…Reflecting remarkable plasticity, CD14 1 myelomonocytic cells efficiently respond to various environmental stimuli, particularly the semi-allograft, which might induce the differentiation of these cells in a tissue-specific manner for immune regulation and host defense responses 2,[27][28][29] . Studies have shown that CD14 1 myelomonocytic cells, which intimately contact the embryo allograft, displayed a unique ability to promote immunotolerance via the induction of Tregs 2 .…”

Section: Discussionmentioning

confidence: 99%

“…As major leukocyte subsets, CD14 1 myelomonocytic cells increase after embryo implantation and closely contact fetal trophoblast cells. Owing to their remarkable plasticity, cytokine production, and functional properties, different subtypes of maternal CD14 1 myelomonocytic cells perform multiple disparate functions during early pregnancy [2][3][4][5] . Maternal CD14 1 myelomonocytic cells have gained increasing attention, as these cells play a multifaceted role during early pregnancy; however, the definition of new subsets and the contribution of each population to the immunological microenvironment of pregnancy are just beginning to emerge.…”

Section: Introductionmentioning

confidence: 99%

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Human trophoblast cells induced MDSCs from peripheral blood CD14+ myelomonocytic cells via elevated levels of CCL2

Zhang

Sun

et al. 2015

Cell Mol Immunol

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Successful human pregnancy requires the maternal immune system to recognize and tolerate the semi-allogeneic fetus. Myeloid-derived suppressor cells (MDSCs), which are capable of inhibiting T-cell responses, are highly increased in the early stages of pregnancy. Although recent reports indicate a role for MDSCs in fetal-maternal tolerance, little is known about the expansion of MDSCs during pregnancy. In the present study, we demonstrated that the trophoblast cell line HTR8/SVneo could instruct peripheral CD14 1 myelomonocytic cells toward a novel subpopulation of MDSCs, denoted as CD14 1 HLA-DR 2/low cells, with suppressive activity and increased expression of IDO1, ARG-1, and COX2. After interaction with HTR8/SVneo cells, CD14 1 myelomonocytic cells secrete high levels of CCL2, promoting the expression of signal transducer and activator of transcription 3. We utilized a neutralizing monoclonal antibody to reveal the prominent role of CCL2 in the induction of CD14 1 HLA-DR 2/low MDSCs. In combination, the results of the present study support a novel role for the cross-talk between the trophoblast cell line HTR8/SVneo and maternal CD14 1 myelomonocytic cells in initiating MDSCs induction, prompting a tolerogenic immune response to ensure a successful pregnancy. Cellular & Molecular Immunology

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Human trophoblast cells induced MDSCs from peripheral blood CD14+ myelomonocytic cells via elevated levels of CCL2

Zhang

Sun

et al. 2015

Cell Mol Immunol

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“…39 Differentiation of CD34 1 cells into CD56 bright NK cells has also been demonstrated in other tissues, such as the lymph nodes. 40 Recently, studies in mice have described two waves of distinct hematopoietic cells in the fetal thymus with potential to develop into NK cells. 65 The different hypotheses regarding the origin of dNK cells are not mutually exclusive.…”

Section: Human Nk Cellsmentioning

confidence: 99%

“…Moreover, iDCs are able to affect the cytokine profile of dNK cells by inducing the IFN-c release of dNK cells. 40 In turn, dNK-derived IFN-c induces the expression of some suppressive molecules, such as indoleamine 2,3-dioxygenase, in decidual DCs, thereby promoting the induction of regulatory T cells in the human decidua (Figure 2b). 60 Similarly, dNK cells are also able to influence DC function during pregnancy.…”

Section: Nk/dc Liaison At the Fetomaternal Interfacementioning

confidence: 99%

Liaison between natural killer cells and dendritic cells in human gestation

et al. 2014

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A successful pregnancy relies on immunological adaptations that allow the fetus to grow and develop in the uterus, despite being recognized by maternal immune cells. Among several immunocompetent cell types present within the human maternal/fetal interface, DC-SIGN 1 dendritic cells (DCs) and CD56 1 natural killer (NK) cells are of major importance for early pregnancy maintenance, not only generating maternal immunological tolerance but also regulating stromal cell differentiation. Previous reports show the presence of NK-DC cell conjugates in first trimester human decidua, suggesting that these cells may play a role in the modulation of the local immune response within the uterus. While effective immunity is necessary to protect the mother from harmful pathogens, some form of tolerance must be activated to avoid an immune response against fetal antigens. This review article discusses current evidence concerning the functions of DC and NK cells in pregnancy and their liaison in human decidua.

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“…18 It was reported that the interaction of dNK and CD14 1 cells lead to CD4 1 CD25 1 regulatory T (Treg) cells induction and immunosuppression. 19 Moreover, a recent study showed that CD56 bright CD27 1 NK cells promote immune tolerance and successful pregnancy through IFN-c secretion, thereby inhibiting inflammatory TH17 cells. 20 Similar to the TH1 and TH2 subsets of CD4 1 T cells, NK cells are divided into NK1 and NK2 subpopulations based on their cytokine secretion profiles.…”

Section: Introductionmentioning

confidence: 99%

CD56brightCD25+ NK cells are preferentially recruited to the maternal/fetal interface in early human pregnancy

Piao

et al. 2014

Cell Mol Immunol

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Decidual natural killer (dNK) cells are believed to be critical for maintaining maternal/fetal tolerance and regulating placental vascular remodeling based upon their abundance and unique phenotype during early pregnancy. However, the mechanism for how the dNK cells play such important roles in successful pregnancy remains undefined. Here, we identified a subtype of dNK cells characterized as having a CD3 2 CD56 bright CD25 1 phenotype. We found that CD56 bright CD25 1 NK cells preferentially localize to the maternal/fetal interface during early human pregnancy. CD25 1 dNK cells account for approximately 75% of CD25-expressing decidual immune cells (DICs). However, less than 5% of CD25-positive peripheral blood mononuclear cells are CD25 1 NK cells. Furthermore, CD25 1 and CD25 2 dNK cells exhibit distinct phenotypes: CD25 1 dNK cells display a more activated phenotype and greater cytokine-secreting capacity. Interestingly, coculture of peripheral NK (pNK) cells with primary trophoblasts upregulates the percentage of CD25-expressing pNK cells, resulting in increased expression of activation markers and cytokine production by pNK cells. In addition, we demonstrated that the CXCL12/CXCR4 axis is crucial for the recruitment of CD25 1 dNK cells and contributes to the accumulation of CD3 2 CD56 bright CD25 1 dNK cells at the maternal/fetal interface. Thus, our data reveal that the crosstalk between trophoblasts and pNK cells leads to the accumulation of CD3 2 CD56 bright CD25 1 dNK cells, which exert a regulating effect at the maternal/fetal interface.

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Crosstalk between decidual NK and CD14 ⁺ myelomonocytic cells results in induction of Tregs and immunosuppression

Cited by 213 publications

References 56 publications

Human trophoblast cells induced MDSCs from peripheral blood CD14+ myelomonocytic cells via elevated levels of CCL2

Human trophoblast cells induced MDSCs from peripheral blood CD14+ myelomonocytic cells via elevated levels of CCL2

Liaison between natural killer cells and dendritic cells in human gestation

CD56brightCD25+ NK cells are preferentially recruited to the maternal/fetal interface in early human pregnancy

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Crosstalk between decidual NK and CD14 + myelomonocytic cells results in induction of Tregs and immunosuppression

Cited by 213 publications

References 56 publications

Human trophoblast cells induced MDSCs from peripheral blood CD14+ myelomonocytic cells via elevated levels of CCL2

Human trophoblast cells induced MDSCs from peripheral blood CD14+ myelomonocytic cells via elevated levels of CCL2

Liaison between natural killer cells and dendritic cells in human gestation

CD56brightCD25+ NK cells are preferentially recruited to the maternal/fetal interface in early human pregnancy

Contact Info

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Crosstalk between decidual NK and CD14 ⁺ myelomonocytic cells results in induction of Tregs and immunosuppression