雅普1
河马信号通路
生物
癌症研究
效应器
细胞生物学
背景(考古学)
下调和上调
转录因子
基因
遗传学
古生物学
作者
Shun Uemura,Masayuki Yamashita,Kazumasa Aoyama,Takako Yokomizo‐Nakano,Motohiko Oshima,Miki Nishio,Masayoshi Masuko,Jun Takizawa,Hirohito Sone,Yasuhiro Yamada,Akira Suzuki,Atsushi Iwama
标识
DOI:10.1016/j.bbrc.2022.06.050
摘要
Radiation therapy is one of the major treatment modalities for patients with cancers. However, ionizing radiation (IR) damages not only cancer cells but also the surrounding vascular endothelial cells (ECs). Hippo pathway effector genes Yap1 and Taz are the two transcriptional coactivators that have crucial roles in tissue homeostasis and vascular integrity in various organs. However, their function in adult ECs at the steady state and after IR is poorly understood. Here, we report sex- and context-dependent roles of endothelial YAP1/TAZ in maintaining vascular integrity and organismal survival. EC-specific Yap1/Taz deletion compromised systemic vascular integrity, resulting in lethal circulation failure preferentially in male mice. Furthermore, EC-specific Yap1/Taz deletion induced acute lethality upon sublethal IR that was closely associated with exacerbated systemic vascular dysfunction and circulation failure. Consistent with these findings, RNA-seq analysis revealed downregulation of tight junction genes in Yap1/Taz-deleted ECs. Collectively, our findings highlight the importance of endothelial YAP1/TAZ for maintaining adult vascular function, which may provide clinical implications for preventing organ injury after radiation therapy.
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