The activation of cGAS‐STING pathway causes abnormal uterine receptivity in aged mice

Author:

Chen Si‐Ting123,Shi Wen‐Wen3,Ran Feng12,Liu Cheng‐Kan3,Luo Hui‐Na3,Wu Li‐Juan12,Wu Ying3,Zhang Tong‐Tong3,Yang Zeng‐Ming123ORCID

Affiliation:

1. Key Laboratory of Plateau Mountain Animal Genetics, Breeding and Reproduction, Ministry of Education Guizhou University Guiyang China

2. College of Animal Science Guizhou University Guiyang China

3. College of Veterinary Medicine South China Agricultural University Guangzhou China

Abstract

AbstractMaternal age is one of the most important factors affecting the success of maternal pregnancy. Uterine aging is the leading cause of pregnancy failure in older women. However, how uterine aging affects uterine receptivity and decidualization is unclear. In this study, naturally aged one‐year‐old female mice were used to investigate effects of maternal age on embryo implantation during early pregnancy. In our study, we found abnormal uterine receptivity in aged mice. Aged mouse uterus indicates a decrease in nuclear LAMIN A, and an increase in PRELAMIN A and PROGERIN. In aged mouse uterus, double‐stranded DNA (dsDNA) in cytoplasmic fraction is significantly increased. PROGERIN overexpression in mouse uterine epithelial cells and epithelial organoids leads to nuclear DNA leakage and impaired uterine receptivity. DNase I, DNase II, and TREX1 are obviously reduced in aged mouse uterus. Treatments with foreign DNA or STING agonist significantly downregulate uterine receptivity markers and activate cGAS‐STING pathway. Uterine estrogen (E2) concentration is significantly increased in aged mice. After ovariectomized mice are treated with a high level of E2, there are significant increase of PROGERIN and cytoplasmic DNA, and activation of cGAS‐STING pathway. CD14 is significantly increased in aged uterus. Intrauterine CD14 injection inhibits embryo implantation. In vitro CD14 treatment of cultured epithelial cells or epithelial organoids decreases uterine receptivity. Uterine abnormality in aged mouse can be partially rescued by STING inhibitor. In conclusion, uterine PROGERIN increase in aged mouse uterus results in cytoplasmic DNA accumulation and cGAS‐STING pathway activation. CD14 secretion in aged uterus impairs uterine receptivity.

Publisher

Wiley

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