| Literature DB >> 28525591 |
Mahiro Egashira1,2, Yasushi Hirota1,3, Ryoko Shimizu-Hirota4, Tomoko Saito-Fujita1, Hirofumi Haraguchi1, Leona Matsumoto1, Mitsunori Matsuo1, Takehiro Hiraoka1, Tomoki Tanaka1, Shun Akaeda1, Chiaki Takehisa1, Mayuko Saito-Kanatani1, Kei-Ichiro Maeda2, Tomoyuki Fujii1, Yutaka Osuga1.
Abstract
Cellular senescence, defined as an irreversible cell cycle arrest, exacerbates the tissue microenvironment. Our previous study demonstrated that mouse uterine senescent cells were physiologically increased according to gestational days and that their abnormal accumulation was linked to the onset of preterm delivery. We hypothesized that there is a mechanism for removal of senescent cells after parturition to maintain uterine function. In the current study, we noted abundant uterine senescent cells and their gradual disappearance in wild-type postpartum mice. F4/80+ macrophages were present specifically around the area rich in senescent cells. Depletion of macrophages in the postpartum mice using anti-F4/80 antibody enlarged the area of senescent cells in the uterus. We also found excessive uterine senescent cells and decreased second pregnancy success rate in a preterm birth model using uterine p53-deleted mice. Furthermore, a decrease in F4/80+ cells and an increase in CD11b+ cells with a senescence-associated inflammatory microenvironment were observed in the p53-deleted uterus, suggesting that uterine p53 deficiency affects distribution of the macrophage subpopulation, interferes with senescence clearance, and promotes senescence-induced inflammation. These findings indicate that the macrophage is a key player in the clearance of uterine senescent cells to maintain postpartum uterine function.Entities:
Mesh:
Substances:
Year: 2017 PMID: 28525591 DOI: 10.1210/en.2016-1886
Source DB: PubMed Journal: Endocrinology ISSN: 0013-7227 Impact factor: 4.736