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1 September 2008 Expression and Function of PDCD1 at the Human Maternal-Fetal Interface
Elizabeth S. Taglauer, Ann S. Trikhacheva, Joyce G. Slusser, Margaret G. Petroff
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Abstract

The failure to reject the semiallogenic fetus by maternal T lymphocytes suggests that potent mechanisms regulate these cells. PDCD1 is a CD28 family receptor expressed by T cells, and its ligand CD274 is strongly expressed by trophoblast cells of the human placenta. In this study, we examined whether human maternal T cells express PDCD1. Immunofluorescence examination of uterine tissues revealed PDCD1 expression on CD3 cells was low in nonpregnant endometrium but increased in first-trimester decidua and remained elevated in term decidua (P < 0.05). In addition, higher relative proportions of term decidual CD8bright, CD4 , and regulatory T cells expressed PDCD1 in comparison to autologous peripheral blood (P < 0.05). Term decidual T cells also expressed full-length and soluble PDCD1 mRNA isoforms more abundantly than their peripheral blood counterparts (P ≤ 0.05). We also examined the effects of PDCD1:CD274 interactions in decidual T cells. Jar choriocarcinoma cells were transfected with CD274 and cocultured with activated decidual CD4 or CD8bright T cells for 72 h followed by analysis of cytokine concentration and decidual T cell apoptosis. Compared with empty vector-transfected cells, CD274-transfected Jar cells caused a significant suppression of interferon gamma and tumor necrosis factor alpha production by CD4 (P < 0.05) but not CD8bright T cells, while having no effect on secretion of IL10 or T cell apoptosis. These results suggest that the PDCD1:CD274 pathway functions in modification of maternal decidual lymphocyte cytokine secretion during pregnancy.

Elizabeth S. Taglauer, Ann S. Trikhacheva, Joyce G. Slusser, and Margaret G. Petroff "Expression and Function of PDCD1 at the Human Maternal-Fetal Interface," Biology of Reproduction 79(3), 562-569, (1 September 2008). https://doi.org/10.1095/biolreprod.107.066324
Received: 25 October 2007; Accepted: 1 May 2008; Published: 1 September 2008
KEYWORDS
B7-H1
CD274
CD279
decidua
PD-1
PDCD1
PDL1
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