Th1- and Th2-like cytokine production by first trimester decidual large granular lymphocytes is influenced by HLA-G and HLA-E

Rieger, Lorenz; Hofmeister, Valeska; Probe, Christine; Dietl, Johannes; Weiss, E.H.; Steck, Theodore L.; Kämmerer, Ulrike

doi:10.1093/molehr/8.3.255

Cited by 68 publications

(46 citation statements)

References 21 publications

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“…Thus, some disease states may mimic the physiological inflammation associated with pregnancy. Numerous cytokines and chemokines, including GM-CSF, IFN-g, and TNF-a, are produced by the decidua (53,54). In tumors, these cytokines and growth factors are known to upregulate neutrophil expression of CD191 and CD195, and to prime neutrophil migration toward CC chemokines, such as CCL2-5 (55-57).…”

Section: Il2rgmentioning

confidence: 99%

Identification of a Novel Neutrophil Population: Proangiogenic Granulocytes in Second-Trimester Human Decidua

Amsalem

Kwan

Hazan

et al. 2014

The Journal of Immunology

101

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The maternal leukocytes of the first-trimester decidua play a fundamental role in implantation and early development of the fetus and placenta, yet little is known regarding the second-trimester decidual environment. Our multicolor flow cytometric analyses of human decidual leukocytes detected an elevation in tissue resident neutrophils in the second trimester. These cells in both human and murine samples were spatially restricted to decidua basalis. In comparison with peripheral blood neutrophils (PMNs), the decidual neutrophils expressed high levels of neutrophil activation markers and the angiogenesis-related proteins: vascular endothelial growth factor-A, Arginase-1, and CCL2, similarly shown in tumor-associated neutrophils. Functional in vitro assays showed that second-trimester human decidua conditioned medium stimulated transendothelial PMN invasion, upregulated VEGFA, ARG1, CCL2, and ICAM1 mRNA levels, and increased PMN-driven in vitro angiogenesis in a CXCL8-dependent manner. This study identified a novel neutrophil population with a physiological, angiogenic role in human decidua.

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Section: Il2rgmentioning

confidence: 99%

Identification of a Novel Neutrophil Population: Proangiogenic Granulocytes in Second-Trimester Human Decidua

Amsalem

Kwan

Hazan

et al. 2014

The Journal of Immunology

101

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“…Decidual T cells can produce cytokines including interleukin (IL)-3, IL-4, transforming growth factor (TGF)-b 1 , TNF-a and interferon (IFN)-g [42][43][44][45] and it has been suggested that deficient production by decidual T cells of cytokines, such as IL-4 and LIF, may lead to pregnancy failure [47]. Recently, the non-classical class I HLA-G and HLA-E molecules, both of which are expressed by fetal trophoblast cells, have been reported to suppress production by isolated first-trimester uterine NK cells of cytokines including IL-10, IL-13, TNF-a, granulocyte macrophage colony-stimulating factor (GM-CSF) and IFN-g [49]. Whether HLA-G and HLA-E regulate the production of cytokines by decidual T cells and macrophages is unknown.…”

Section: Discussionmentioning

confidence: 99%

No evidence for apoptosis of decidual leucocytes in normal and molar pregnancy: implications for immune privilege

Pongcharoen

Bulmer²,

Searle

2004

Clinical and Experimental Immunology

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SUMMARYComplete hydatidiform moles are totally paternally derived and represent complete allografts that might be expected to provoke maternal immune rejection. Our previous and other studies have shown expression of Fas by increased numbers of activated decidual CD4 + T cells in both complete and partial molar pregnancy as well as increased FasL + expression by molar trophoblasts compared with trophoblasts in normal pregnancies. As the Fas/FasL system represents a major apoptotic pathway that can play a role in immune privilege, the aim of this study was to investigate whether apoptosis of decidual immune cells, particularly T cells, could be responsible for maternal immune tolerance in molar pregnancy. Using terminal deoxynucleotidyl transferase (TdT)-mediated nick end-labelling (TUNEL), a significant increase in TUNEL + cells was demonstrated in decidua associated with partial ( P = 0·0052) and complete ( P = 0·0096) hydatidiform mole compared with normal early pregnancy. Co-labelling immunoperoxidase studies showed that the TUNEL + cells in both normal and molar pregnancies were not activated CD45RO + immune cells, CD3 + T cells, CD56 + uterine natural killer (NK) cells or CD14 + CD68 + macrophages. Double immunohistochemical labelling with antiactive caspase-3 and leucocyte markers confirmed the lack of leucocyte apoptosis. Double immunostaining with anticytokeratin to detect trophoblast and M30 CytoDeath, which detects a neoepitope of cytokeratin 18 revealed after caspase-mediated cleavage, revealed apoptotic extravillous trophoblast cells within decidual tissue. We conclude that there is no evidence that apoptosis of decidual leucocytes plays a role in maintaining maternal tolerance in either normal or molar pregnancy.

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“…proposed to be involved in the modulation of maternal immune responses and has for instance been shown to inhibit cytokine production and reduce NK cell cytotoxicity, to eliminate activated cytotoxic CD8 + T cells and to induce production of TGF-β by APCs (Rieger et al, 2002;Hunt et al, 2005). Although less pronounced, HLA-E has also been shown to inhibit NK cell cytotoxicity (King et al, 2000a).…”

Section: Immune Regulation During Pregnancymentioning

confidence: 99%

Immune regulation at the fetal‐maternal interface with focus on decidual macrophages

Svensson‐Arvelund¹

2015

Linköping University Medical Dissertations

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A successful pregnancy requires that the maternal immune system adapts to tolerate the semi-allogeneic fetal-placental unit. This adaptation mainly occurs locally, i.e. at the fetal-maternal interface, where fetal-derived tissues come into close contact with maternal cells in the uterine endometrium (called decidua during pregnancy). decidual macrophages preferentially secreted the monocyte-and Treg cell-associated chemokines CCL2 and CCL18, while Th1-, Th2-and Th17-related chemokines were produced at low levels. These results suggest that decidual macrophages contribute to create the unique decidual cell composition and a tolerogenic immune environment that is compatible with fetal development. Further, by comparing decidual macrophages with different in vitro macrophage subsets, we showed that M-CSF and

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Th1- and Th2-like cytokine production by first trimester decidual large granular lymphocytes is influenced by HLA-G and HLA-E

Cited by 68 publications

References 21 publications

Identification of a Novel Neutrophil Population: Proangiogenic Granulocytes in Second-Trimester Human Decidua

Identification of a Novel Neutrophil Population: Proangiogenic Granulocytes in Second-Trimester Human Decidua

No evidence for apoptosis of decidual leucocytes in normal and molar pregnancy: implications for immune privilege

Immune regulation at the fetal‐maternal interface with focus on decidual macrophages

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