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Retinoblastoma protein promotes uterine epithelial cell cycle arrest and necroptosis for embryo invasion
Authors:Shun Akaeda  Yasushi Hirota  Yamato Fukui  Shizu Aikawa  Ryoko Shimizu&#x;Hirota  Tetsuaki Kaku  Mona Gebril  Tomoyuki Hirata  Takehiro Hiraoka  Mitsunori Matsuo  Hirofumi Haraguchi  Mayuko Saito&#x;Kanatani  Norihiko Takeda  Tomoyuki Fujii  Yutaka Osuga
Institution:1. Department of Obstetrics and Gynecology, Graduate School of Medicine, The University of Tokyo, Tokyo Japan ; 2. Frontier Outstanding Research for Clinical Empowerment (FORCE), Japan Agency for Medical Research and Development (AMED), Tokyo Japan ; 3. Department of Internal Medicine, Center of Preventive Medicine, School of Medicine, Keio University, Tokyo Japan ; 4. Center for Molecular Medicine, Jichi Medical University, Shimotuke Tochigi, Japan
Abstract:Retinoblastoma protein (RB) encoded by Rb1 is a prominent inducer of cell cycle arrest (CCA). The hormone progesterone (P4) promotes CCA in the uterine epithelium and previous studies indicated that P4 activates RB by reducing the phosphorylated, inactive form of RB. Here, we show that embryo implantation is impaired in uterine‐specific Rb1 knockout mice. We observe persistent cell proliferation of the Rb1‐deficient uterine epithelium until embryo attachment, loss of epithelial necroptosis, and trophoblast phagocytosis, which correlates with subsequent embryo invasion failure, indicating that Rb1‐induced CCA and necroptosis of uterine epithelium are involved in embryo invasion. Pre‐implantation P4 supplementation is sufficient to restore these defects and embryo invasion. In Rb1‐deficient uterine epithelial cells, TNFα‐primed necroptosis is impaired, which is rescued by the treatment with a CCA inducer thymidine or P4 through the upregulation of TNF receptor type 2. TNFα is expressed in the luminal epithelium and the embryo at the embryo attachment site. These results provide evidence that uterine Rb1‐induced CCA is involved in TNFα‐primed epithelial necroptosis at the implantation site for successful embryo invasion.
Keywords:embryo implantation  progesterone  TNFα  signaling  trophoblast phagocytosis  uterine luminal epithelium
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