Regulatory T cells are paramount effectors in progesterone regulation of embryo implantation and fetal growth
Ella S. Green, Lachlan M. Moldenhauer, Holly M. Groome, David J. Sharkey, Peck Y. Chin, Alison S. Care, Rebecca L. Robker, Shaun R. McColl, Sarah A. Robertson
Ella S. Green, Lachlan M. Moldenhauer, Holly M. Groome, David J. Sharkey, Peck Y. Chin, Alison S. Care, Rebecca L. Robker, Shaun R. McColl, Sarah A. Robertson
View: Text | PDF
Research Article Reproductive biology

Regulatory T cells are paramount effectors in progesterone regulation of embryo implantation and fetal growth

Abstract

Progesterone (P4) is essential for embryo implantation, but the extent to which the pro-gestational effects of P4 depend on the maternal immune compartment is unknown. Here, we investigate whether regulatory T cells (Treg cells) act to mediate luteal phase P4 effects on uterine receptivity in mice. P4 antagonist RU486 administered to mice on days 1.5 and 3.5 postcoitum to model luteal phase P4 deficiency caused fewer CD4+Foxp3+ Treg cells and impaired Treg functional competence, along with dysfunctional uterine vascular remodeling and perturbed placental development in midgestation. These effects were linked with fetal loss and fetal growth restriction, accompanied by a Th1/CD8-skewed T cell profile. Adoptive transfer at implantation of Treg cells — but not conventional T cells — alleviated fetal loss and fetal growth restriction by mitigating adverse effects of reduced P4 signaling on uterine blood vessel remodeling and placental structure and by restoring maternal T cell imbalance. These findings demonstrate an essential role for Treg cells in mediating P4 effects at implantation and indicate that Treg cells are a sensitive and critical effector mechanism through which P4 drives uterine receptivity to support robust placental development and fetal growth.

Authors

Ella S. Green, Lachlan M. Moldenhauer, Holly M. Groome, David J. Sharkey, Peck Y. Chin, Alison S. Care, Rebecca L. Robker, Shaun R. McColl, Sarah A. Robertson

×

Figure 6

Treg cell transfer mitigates T cell imbalance in late gestation caused by impaired luteal phase P4 signaling.

Options: View larger image (or click on image) Download as PowerPoint
Treg cell transfer mitigates T cell imbalance in late gestation caused b...
Female B6 mice were mated to BALB/c males and administered RU486 (1 mg/kg) or vehicle (control) on 1.5 and 3.5 dpc. On 3.5 dpc, approximately 8 hours following the final RU486 dose, females were injected i.v. with 2 × 105 Treg cells (CD4+CD25+), Tconv cells (CD4+CD25), or vehicle control (PBS), and then CD4+ T cells in udLNs recovered on 18.5 dpc were analyzed by flow cytometry. (A) Total cell count, and number and proportion of CD4+ T cells, for each group in control mice and mice treated with RU486, RU486+Treg cells, and RU486+Tconv cells. (B) Total Treg cell number and Nrp1+ Treg cell number. (C) Proportion of Foxp3+ Treg cells (%CD4+) and proportion of Nrp1+ (%Treg) per group. (AC) n = 6–7 pregnant dams/group. Data shown as mean ± SEM with individual mice indicated by symbols, analyzed by 1-way ANOVA with Sidak’s post hoc t test, *P < 0.05, **P < 0.01.