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A common allele increases endometrial Wnt4 expression, with antagonistic implications for pregnancy, reproductive cancers, and endometriosis

Mihaela Pavličev, Caitlin E. McDonough-Goldstein, Andreja Moset Zupan, Lisa M. Muglia, Yueh‐Chiang Hu, Fansheng Kong, Nagendra Monangi, Gulay Dagdas, N. Župančič, Jamie Maziarz, Débora Sinner, Ge Zhang, Günter P. Wagner, Louis J. Muglia

2024Nature Communications12 citationsDOIOpen Access PDF

Abstract

The common human SNP rs3820282 is associated with multiple phenotypes including gestational length and likelihood of endometriosis and cancer, presenting a paradigmatic pleiotropic variant. Deleterious pleiotropic mutations cause the co-occurrence of disorders either within individuals, or across population. When adverse and advantageous effects are combined, pleiotropy can maintain high population frequencies of deleterious alleles. To reveal the causal molecular mechanisms of this pleiotropic SNP, we introduced this substitution into the mouse genome by CRISPR/Cas 9. Previous work showed that rs3820282 introduces a high-affinity estrogen receptor alpha-binding site at the Wnt4 locus. Here, we show that this mutation upregulates Wnt4 transcription in endometrial stroma, following the preovulatory estrogen peak. Effects on uterine transcription include downregulation of epithelial proliferation and induction of progesterone-regulated pro-implantation genes. We propose that these changes increase uterine permissiveness to embryo invasion, whereas they decrease resistance to invasion by cancer and endometriotic foci in other estrogen-responsive tissues.

Topics & Concepts

BiologyWNT4PopulationEndometriosisAlleleEstrogen receptorProgesterone receptorDecidualizationCancer researchEndometrial cancerGeneticsGeneEmbryoInternal medicineCancerBreast cancerWnt signaling pathwayMedicineEnvironmental healthReproductive System and PregnancyEndometriosis Research and TreatmentReproductive Biology and Fertility