Dendritic cell entrapment within the pregnant uterus inhibits immune surveillance of the maternal/fetal interface in mice
Mary K. Collins, … , Chin-Siean Tay, Adrian Erlebacher
Mary K. Collins, … , Chin-Siean Tay, Adrian Erlebacher
Published June 22, 2009
Citation Information: J Clin Invest. 2009;119(7):2062-2073. https://doi.org/10.1172/JCI38714.
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Research Article

Dendritic cell entrapment within the pregnant uterus inhibits immune surveillance of the maternal/fetal interface in mice

Abstract

Embryo implantation induces formation of the decidua, a stromal cell–derived structure that encases the fetus and placenta. Using the mouse as a model organism, we have found that this tissue reaction prevents DCs stationed at the maternal/fetal interface from migrating to the lymphatic vessels of the uterus and thus reaching the draining lymph nodes. Strikingly, decidual DCs remained immobile even after being stimulated with LPS and exhibiting responsiveness to CCL21, the chemokine that drives DC entry into lymphatic vessels. An analysis of maternal T cell reactivity toward a surrogate fetal/placental antigen furthermore revealed that regional T cell responses toward the fetus and placenta were driven by passive antigen transport and thus the tolerogenic mode of antigen presentation that predominates when there is negligible input from tissue-resident DCs. Indeed, the lack of involvement of tissue-resident DCs in the T cell response to the fetal allograft starkly contrasts with their prominent role in organ transplant rejection. Our results suggest that DC entrapment within the decidua minimizes immunogenic T cell exposure to fetal/placental antigens and raise the possibility that impaired development or function of the human decidua, which unlike that of the mouse contains lymphatic vessels, might lead to pathological T cell activation during pregnancy.

Authors

Mary K. Collins, Chin-Siean Tay, Adrian Erlebacher

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Figure 6

Lymphatic distribution and CCL21 expression in the nonpregnant and pregnant uterus.

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Lymphatic distribution and CCL21 expression in the nonpregnant and pregn...
Nonpregnant uteri (A, B, E, and F; scale bar: 0.5 mm) and E10.5 implantation sites (C, D, G, and H; scale bar: 1 mm) were stained with antibodies against the lymphatic vessel marker LYVE-1 (A, C, E, and G) or CCL21 (B, D, F, and H) and counterstained with DAPI. Color images are shown in AD; black and white images without the DAPI channel are shown in EH for clarity. The orange dashed lines in A and C demarcate the myometrium from endometrium and the myometrium from decidua, respectively. The white dashed line in C demarcates the placenta from decidua. In addition to lymphatic vessels, LYVE-1 is also expressed by yolk sac endothelial cells. The asterisks in C indicate some staining artifacts caused by tissue folding; the asterisk in D indicates some nonspecific staining also seen in the absence of primary antibody. Staining intensities were subjected to nonlinear adjustments so that structures would be visible at low magnification.