Stromal Pbrm1 mediates chromatin remodeling necessary for embryo implantation in the mouse uterus
Qiliang Xin, … , Guoyun Yu, Jurrien Dean
Qiliang Xin, … , Guoyun Yu, Jurrien Dean
Published March 1, 2024
Citation Information: J Clin Invest. 2024;134(5):e174194. https://doi.org/10.1172/JCI174194.
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Research Article Endocrinology Reproductive biology

Stromal Pbrm1 mediates chromatin remodeling necessary for embryo implantation in the mouse uterus

Abstract

Early gestational loss occurs in approximately 20% of all clinically recognized human pregnancies and is an important cause of morbidity. Either embryonic or maternal defects can cause loss, but a functioning and receptive uterine endometrium is crucial for embryo implantation. We report that the switch/sucrose nonfermentable (SWI/SNF) remodeling complex containing polybromo-1 (PBRM1) and Brahma-related gene 1 (BRG1) is essential for implantation of the embryonic blastocyst on the wall of the uterus in mice. Although preimplantation development is unaffected, conditional ablation of Pbrm1 in uterine stromal cells disrupts progesterone pathways and uterine receptivity. Heart and neural crest derivatives expressed 2 (Hand2) encodes a basic helix-loop-helix (bHLH) transcription factor required for embryo implantation. We identify an enhancer of the Hand2 gene in stromal cells that requires PBRM1 for epigenetic histone modifications/coactivator recruitment and looping with the promoter. In Pbrm1cKO mice, perturbation of chromatin assembly at the promoter and enhancer sites compromises Hand2 transcription, adversely affects fibroblast growth factor signaling pathways, prevents normal stromal-epithelial crosstalk, and disrupts embryo implantation. The mutant female mice are infertile and provide insight into potential causes of early pregnancy loss in humans.

Authors

Qiliang Xin, Iris Feng, Guoyun Yu, Jurrien Dean

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Figure 5

Uterine-specific depletion of Brg1 results in embryo implantation failure and female infertility.

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Uterine-specific depletion of Brg1 results in embryo implantation failur...
(A) Immunohistochemical staining documents a spatiotemporal expression of BRG1 in WT uteri on D1, D4, and D5 of pregnancy. Scale bar: 100 mm. (BD) RT-qPCR (B), immunoblotting (C), and immunohistochemical images (D) of Brg1 mRNA and BRG1 protein levels in D4 uteri from Brg1fl/fl and Brg1fl/fl/PRIRES-cre/+ mice. Values are normalized to Gapdh expression and represented as mean ± SEM (n = 4). ***P < 0.001, independent-sample Student’s t test. β-actin, load control. Scale bar: 100 mm. (E) Number of ovulated eggs in Brg1fl/fl and Brg1fl/fl/PRIRES-cre/+ mice. Numbers within the bars indicate numbers of mice tested. (F) Average litter sizes of Brg1fl/fl and Brg1fl/fl/PRIRES-cre/+ female mice. Numbers within the bars indicate numbers of mice tested. Data are represented as mean ± SEM. ***P < 0.001, independent-sample Student’s t test. (G and H) Representative images of normal embryo morphology from D5 (G) and D6 (H) pregnant Brg1fl/fl/PRIRES-cre/+ mice, exhibiting embryo implantation failure in the uteri beyond D5. Numbers within the bars indicate numbers of mice with implantation sites per total tested mice. Data are represented as mean ± SEM. **P < 0.01, independent-samples Student’s t test. Scale bars, 1 cm (uterus); 100 mm (embryos). (I and J) Immunofluorescence staining of PCNA and HAND2 document aberrant epithelial proliferation and impaired uterine receptivity in Brg1fl/fl/PRIRES-cre/+ females on D4. Scale bars: 100 mm.