Fetal and maternal NLRP3 signaling is required for preterm labor and birth
Kenichiro Motomura, … , Adi L. Tarca, Nardhy Gomez-Lopez
Kenichiro Motomura, … , Adi L. Tarca, Nardhy Gomez-Lopez
Published August 22, 2022
Citation Information: JCI Insight. 2022;7(16):e158238. https://doi.org/10.1172/jci.insight.158238.
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Research Article Immunology Reproductive biology

Fetal and maternal NLRP3 signaling is required for preterm labor and birth

Abstract

Preterm birth is the leading cause of neonatal morbidity and mortality worldwide. One of every 4 preterm neonates is born to a mother with intra-amniotic inflammation driven by invading bacteria. However, the molecular mechanisms underlying this hostile immune response remain unclear. Here, we used a translationally relevant model of preterm birth in Nlrp3-deficient and -sufficient pregnant mice to identify what we believe is a previously unknown dual role for the NLRP3 pathway in the fetal and maternal signaling required for the premature onset of the labor cascade leading to fetal injury and neonatal death. Specifically, the NLRP3 sensor molecule and/or inflammasome is essential for triggering intra-amniotic and decidual inflammation, fetal membrane activation, uterine contractility, and cervical dilation. NLRP3 also regulates the functional status of neutrophils and macrophages in the uterus and decidua, without altering their influx, as well as maternal systemic inflammation. Finally, both embryo transfer experimentation and heterozygous mating systems provided mechanistic evidence showing that NLRP3 signaling in both the fetus and the mother is required for the premature activation of the labor cascade. These data provide insights into the mechanisms of fetal-maternal dialog in the syndrome of preterm labor and indicate that targeting the NLRP3 pathway could prevent adverse perinatal outcomes.

Authors

Kenichiro Motomura, Roberto Romero, Jose Galaz, Li Tao, Valeria Garcia-Flores, Yi Xu, Bogdan Done, Marcia Arenas-Hernandez, Derek Miller, Pedro Gutierrez-Contreras, Marcelo Farias-Jofre, Siddhesh Aras, Lawrence I. Grossman, Adi L. Tarca, Nardhy Gomez-Lopez

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Figure 6

Nlrp3 deficiency protects against preterm birth by limiting decidual inflammation.

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Nlrp3 deficiency protects against preterm birth by limiting decidual in...
(A) Pregnant Nlrp3+/+ and Nlrp3–/– mice were intra-amniotically injected with LPS (100 ng/25 μL) or PBS on 16.5 days post coitum (dpc). We collected the decidua basalis on 17.5 dpc. The spatial localization of the murine decidua is shown. (B) Heatmap visualization of inflammatory gene expression in the decidua (n = 13–15 per group). (C) Expression of the inflammation-associated genes (n = 13–15 per group). (D) Immunoblotting of pro-CASP and CASP-1 p20 in the decidua (n = 6 per group). The expression was normalized by ACTB and shown as relative quantification. (E) Concentrations of total IL-1β in the decidua. Values were adjusted by the total protein concentration in each sample (n = 8–9 per group). (F) Immunoblotting of mature IL-1β in decidual tissue lysates immunoprecipitated with anti–IL-1β antibody (n = 3 per group). (G) Representative immunofluorescence images showing the expression of neutrophil elastase (NE) in the decidua (n = 5–7 per group). All images were taken at 200× original magnification. Scale bars represent 20 μm. Inset images show isotype control staining from the same case. (H) Immunoblotting of 2-chain NE in decidual tissue lysates (n = 6 per group). Data are shown as box-and-whisker plots where midlines indicate medians, boxes indicate interquartile ranges, and whiskers indicate minimum and maximum values. The P values of the comparisons between PBS- and LPS-injected dams of each genotype were determined by Mann-Whitney U test. *P < 0.05; **P < 0.01; ***P < 0.001; (+) Ctrl., positive control.