Abstract
Trophoblast cells are unique because they are one of the few mammalian cell types that do not express major histocompatibility complex (MHC) class II antigens, either constitutively or after exposure to IFN-γ. The absence of MHC class II antigen expression on trophoblast cells has been postulated to be one of the essential mechanisms by which the semi-allogeneic fetus evades immune rejection reactions by the maternal immune system. Consistent with this hypothesis, trophoblast cells from the placentas of women suffering from chronic inflammation of unknown etiology and spontaneous recurrent miscarriages have been reported to aberrantly express MHC class II antigens. The lack of MHC class II antigen expression on trophoblast cells is due to silencing of expression of the class II transactivator (CIITA), a transacting factor that is essential for constitutive and IFN-γ-inducible MHC class II gene transcription. Transfection of trophoblast cells with CIITA expression vectors activates both MHC class II and class Ia antigen expression, which confers on trophoblast cells both the ability to activate helper T cells, and sensitivity to lysis by cytotoxic T lymphocytes. Collectively, these studies strongly suggest that stringent silencing of CIITA (and therefore MHC class II) gene expression in trophoblast cells is critical for the prevention of immune rejection responses against the fetus by the maternal immune system. The focus of this review is to summarize studies examining the novel mechanisms by which CIITA is silenced in trophoblast cells. The elucidation of the silencing of CIITA in trophoblast cells may shed light on how the semi-allogeneic fetus evades immune rejection by the maternal immune system during pregnancy.
Highlights
The successful maintenance of the semi-allogeneic mammalian fetus during pregnancy provides an apparent immunological paradox
Silencing of class II transactivator (CIITA) transcription in trophoblast cells is likely to be crucial for successful maintenance of the fetus, and recent studies suggest that the precise mechanism of silencing may be novel
In the absence of IFN-γ, the CIITA PIV is associated with histone deacetylases (HDACs) and is in a closed chromatin conformation in CIITA-inducible cells, and trophoblast cells
Summary
The successful maintenance of the semi-allogeneic mammalian fetus during pregnancy provides an apparent immunological paradox. Transient transfection assays demonstrated that the IFN-γ-responsive CIITA type IV promoter is functionally active in trophoblast cells, despite the fact that the endogenous CIITA gene is not expressed [11,15,42] These results suggested that trophoblast cells contain the transacting DNA binding factors (STAT-1, USF-1 and IRF-1) required for IFN-γinducible CIITA transcription. These data are consistent with a model in which endogenous CIITA transcription in trophoblast cells is repressed by epigenetic mechanism(s) which maintain a closed chromatin conformation, such as promoter methylation and/or the insufficient acetylation of histones. It http://www.rbej.com/content/2/1/52 remains to be determined whether this is the case for the trophoblast-specific utRNA described by Peyman [47] and Geirsson et al [48,49]
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