| Literature DB >> 30429548 |
Roser Vento-Tormo1,2, Mirjana Efremova1, Muzlifah Haniffa3,4,5, Ashley Moffett6,7, Sarah A Teichmann8,9,10, Rachel A Botting11, Margherita Y Turco2,12,13, Miquel Vento-Tormo14, Kerstin B Meyer1, Jong-Eun Park1, Emily Stephenson11, Krzysztof Polański1, Angela Goncalves1,15, Lucy Gardner2,12, Staffan Holmqvist16, Johan Henriksson1, Angela Zou1, Andrew M Sharkey2,12, Ben Millar11, Barbara Innes11, Laura Wood1, Anna Wilbrey-Clark1, Rebecca P Payne11, Martin A Ivarsson12, Steve Lisgo17, Andrew Filby11, David H Rowitch16, Judith N Bulmer11, Gavin J Wright1, Michael J T Stubbington1.
Abstract
During early human pregnancy the uterine mucosa transforms into the decidua, into which the fetal placenta implants and where placental trophoblast cells intermingle and communicate with maternal cells. Trophoblast-decidual interactions underlie common diseases of pregnancy, including pre-eclampsia and stillbirth. Here we profile the transcriptomes of about 70,000 single cells from first-trimester placentas with matched maternal blood and decidual cells. The cellular composition of human decidua reveals subsets of perivascular and stromal cells that are located in distinct decidual layers. There are three major subsets of decidual natural killer cells that have distinctive immunomodulatory and chemokine profiles. We develop a repository of ligand-receptor complexes and a statistical tool to predict the cell-type specificity of cell-cell communication via these molecular interactions. Our data identify many regulatory interactions that prevent harmful innate or adaptive immune responses in this environment. Our single-cell atlas of the maternal-fetal interface reveals the cellular organization of the decidua and placenta, and the interactions that are critical for placentation and reproductive success.Entities:
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Year: 2018 PMID: 30429548 PMCID: PMC7612850 DOI: 10.1038/s41586-018-0698-6
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 69.504