Successful placentation in human pregnancy is regulated by reciprocal interactions between maternal uterine NK cells and fetal placental trophoblast

滋养层 胎盘形成 胎盘 生物 胎儿 怀孕 细胞生物学 男科 免疫学 医学 遗传学
作者
Qian Li,Andrew Sharkey,Megan A. Sheridan,Elisa Magistrati,Anna Arutyunyan,Oisín Huhn,Carmen Sancho‐Serra,Holly E. Anderson,Naomi McGovern,Laura Esposito,Ridma C. Fernando,Lucy Gardner,Roser Vento‐Tormo,Margherita Y. Turco,Ashley Moffett
标识
DOI:10.1101/2023.06.07.544122
摘要

Summary Fetal growth and development during human pregnancy depends on delivery of adequate maternal oxygen and nutrients to the fetus via the placenta. In humans, the balanced invasion of fetal placental trophoblast cells into the maternal uterine lining, where they interact with uterine natural killer cells (uNK), is thought to be critical for a successful pregnancy but exactly how this influences reproductive outcomes remains undefined. Here, we used our trophoblast organoid model and primary tissue samples to determine how uNK affect placentation. By locating potential interaction axes between primary trophoblast cells and uNK using single cell transcriptomics, and in vitro modelling of these interactions in trophoblast organoids, we identify a uNK-derived cytokine signal that promotes trophoblast differentiation by enhancing epithelial-mesenchymal transition and increasing trophoblast cells at the late stage of the invasive pathway. Moreover, it affects transcriptional programs involved in increasing blood flow, placental access to nutrients, and dampening inflammatory and adaptive immune responses, as well as gene signatures associated with disorders of pregnancy such as pre-eclampsia. Our findings shed new light on how optimal immunological interactions between maternal uNK cells and fetal trophoblast enhance reproductive success.
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