Literature DB >> 24581729

Potentiating maternal immune tolerance in pregnancy: a new challenging role for regulatory T cells.

J Alijotas-Reig1, E Llurba2, J Ma Gris3.   

Abstract

The maternal immune system needs to adapt to tolerate the semi-allogeneic conceptus. Since maternal allo-reactive lymphocytes are not fully depleted, other local/systemic mechanisms play a key role in altering the immune response. The Th1/Th2 cytokine balance is not essential for a pregnancy to be normal. The immune cells, CD4+CD25+Foxp3+, also known as regulatory T cells (Tregs), step in to regulate the allo-reactive Th1 cells. In this review we discuss the role of Tregs in foeto-maternal immune tolerance and in recurrent miscarriage as well as their potential use as a new target for infertility treatment. Animal and human experiments showed Treg cell number and/or function to be diminished in miscarriages. Murine miscarriage can be prevented by transferring Tregs from normal pregnant mice. Tregs at the maternal-fetal interface prevented fetal allo-rejection by creating a "tolerant" microenvironment characterised by the expression of IL-10, TGF-β and haem oxygenase isoform 1 (HO-1) rather than by lowering Th1 cytokines. Tregs increase placental HO-1. In turn, HO-1 may lead to up-regulation of TGF-β, IL-10 and CTLA-4. In vivo experiments showed Tregs sensitisation from paternal antigens to be essential for maternal-fetal tolerance. Tregs increase throughout pregnancy and diminish in late puerperium. Recent data also support the capacity of Tregs to block maternal effector T cells, thereby reducing the maternal-fetal pathological responses to paternal antigens. These findings also permit us to consider new strategies for improving pregnancy outcomes, i.e., anti-TNF blockers and granulocyte-colony stimulating factors as well as novel approaches to therapeutically exploiting Treg + cell memory.
Copyright © 2014 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  Cytokines; Maternal–fetal tolerance; Miscarriages; NK cells/KIR; Regulatory-T lymphocytes; Treatment

Mesh:

Year:  2014        PMID: 24581729     DOI: 10.1016/j.placenta.2014.02.004

Source DB:  PubMed          Journal:  Placenta        ISSN: 0143-4004            Impact factor:   3.481


  42 in total

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3.  The sterile and tolerogenic fetal niche does not restrict the generation of CD4 T memory cells.

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5.  Expression of CD24 and Siglec-10 in first trimester placenta: implications for immune tolerance at the fetal-maternal interface.

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6.  Association between cytokine profile and transcription factors produced by T-cell subsets in early- and late-onset pre-eclampsia.

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Authors:  Renju S Raj; Elizabeth A Bonney; Mark Phillippe
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8.  Sleep Disturbance in Early Pregnancy, but Not Inflammatory Cytokines, May Increase Risk for Adverse Pregnancy Outcomes.

Authors:  Michele L Okun; Vanessa Obetz; Leilani Feliciano
Journal:  Int J Behav Med       Date:  2021-02

Review 9.  From apelin to exercise: emerging therapies for management of hypertension in pregnancy.

Authors:  Jeffrey S Gilbert
Journal:  Hypertens Res       Date:  2017-04-06       Impact factor: 3.872

10.  PD-L1 Expression in Human Placentas and Gestational Trophoblastic Diseases.

Authors:  Emanuela Veras; Robert J Kurman; Tian-Li Wang; Ie-Ming Shih
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