An IGF1-expressing endometrial stromal cell population is associated with human decidualization

蜕膜化 间质细胞 生物 蜕膜 蜕膜细胞 子宫内膜 细胞生物学 滋养层 内科学 内分泌学 癌症研究 胎盘 遗传学 怀孕 医学 胎儿
作者
Jing Shi,Zhen‐Zhen Lai,Hui‐Li Yang,Wen‐Jie Zhou,Xiujuan Zhao,Feng Xie,Songping Liu,Weidong Chen,Tao Zhang,Jiang-Feng Ye,Xiangyu Zhou,Ming‐Qing Li
出处
期刊:BMC Biology [BioMed Central]
卷期号:20 (1) 被引量:6
标识
DOI:10.1186/s12915-022-01483-0
摘要

Decidualization refers to the process of transformation of endometrial stromal fibroblast cells into specialized decidual stromal cells that provide a nutritive and immunoprivileged matrix essential for blastocyst implantation and placental development. Deficiencies in decidualization are associated with a variety of pregnancy disorders, including female infertility, recurrent implantation failure (RIF), and miscarriages. Despite the increasing number of genes reportedly associated with endometrial receptivity and decidualization, the cellular and molecular mechanisms triggering and underlying decidualization remain largely unknown. Here, we analyze single-cell transcriptional profiles of endometrial cells during the window of implantation and decidual cells of early pregnancy, to gains insights on the process of decidualization.We observed a unique IGF1+ stromal cell that may initiate decidualization by single-cell RNA sequencing. We found the IL1B+ stromal cells promote gland degeneration and decidua hemostasis. We defined a subset of NK cells for accelerating decidualization and extravillous trophoblast (EVT) invasion by AREG-IGF1 and AREG-CSF1 regulatory axe. Further analysis indicates that EVT promote decidualization possibly by multiply pathways. Additionally, a systematic repository of cell-cell communication for decidualization was developed. An aberrant ratio conversion of IGF1+ stromal cells to IGF1R+ stromal cells is observed in unexplained RIF patients.Overall, a unique subpopulation of IGF1+ stromal cell is involved in initiating decidualization. Our observations provide deeper insights into the molecular and cellular characterizations of decidualization, and a platform for further development of evaluation of decidualization degree and treatment for decidualization disorder-related diseases.
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