IL-27/Blimp-1 axis regulates the differentiation and function of Tim-3+ Tregs during early pregnancy
Si-Jia Zhao, Xiao-Hui Hu, Xin-Xiu Lin, Yu-Jing Zhang, Jing Wang, Huan Wang, Guang-Shun Gong, Gil Mor, Ai-Hua Liao
Si-Jia Zhao, Xiao-Hui Hu, Xin-Xiu Lin, Yu-Jing Zhang, Jing Wang, Huan Wang, Guang-Shun Gong, Gil Mor, Ai-Hua Liao
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Research Article Immunology Reproductive biology

IL-27/Blimp-1 axis regulates the differentiation and function of Tim-3+ Tregs during early pregnancy

Abstract

Decidual regulatory T cells (Tregs) are essential for successful pregnancy outcome. A subset of Tregs, T cell immunoglobulin and mucin domain-containing protein 3–positive regulatory T cells (TregsTim-3+), plays a central role in the acceptance of the fetus during early stages of normal pregnancy. The molecular mechanism regulating the differentiation and function of TregsTim-3+ is unknown. Here, we investigated the role of the transcription factor B lymphocyte-induced maturation protein 1 (Blimp-1) on decidual TregTim-3+ differentiation. We demonstrated that Blimp-1 enhanced the coexpression of negative costimulatory molecules (Tim-3, T cell immunoreceptor with Ig and ITIM domains, and programmed cell death protein 1) on Tregs and improved their immunosuppressive functions, including increased IL-10 secretion, suppression of effector T cell proliferation, and promotion of macrophage polarization toward the M2 phenotype. Furthermore, we showed that IL-27 regulated the expression of Tim-3 and Blimp-1 through the STAT1 signaling pathway and that transfer of TregsBlimp-1+ into an abortion-prone mouse model effectively reduced embryo absorption rate. We postulated that abnormalities in the IL-27/Blimp-1 axis might be associated with recurrent pregnancy loss (RPL). These findings provided insights for developing more efficient immunotherapies for women with RPL.

Authors

Si-Jia Zhao, Xiao-Hui Hu, Xin-Xiu Lin, Yu-Jing Zhang, Jing Wang, Huan Wang, Guang-Shun Gong, Gil Mor, Ai-Hua Liao

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Figure 7

Impact of TregBlimp-1 transfer on mouse pregnancy outcomes.

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Impact of TregBlimp-1 transfer on mouse pregnancy outcomes. (A) FCM gati...
(A) FCM gating strategy from decidual tissues. (B) Proportions of Tregs and Tim-3+ Tregs in the spleen of each AT group were detected by FCM at GD 13.5 (n = 5). (C) Proportions of Tregs and Tim-3+ Tregs in the inguinal lymph nodes of each AT group were detected by FCM at GD 13.5 (n = 5). (D) Proportions of Tregs and Tim-3+ Tregs in the decidua of each AT group were detected by FCM at GD 13.5 (n = 5). (E) Coexpression of PD-1, Tim-3, CD4, and Foxp3 in the materno-fetal interface was detected using mIHC. The first row shows the placental overall structure in LPS+TregBlimp-1 and LPS+TregIL-27 groups under ×50 original magnification (scale bar: 500 μm). The bottom 2 rows show the placenta in view of ×1,000 original magnification (scale bar: 50 μm). Data are represented as the mean ± SEM via 1-way ANOVA test (BD) and Tukey’s multiple comparisons test between each 2 groups. *P < 0.05, **P < 0.01.