淋巴系统
压电1
淋巴管内皮
下调和上调
淋巴管新生
淋巴管
细胞生物学
化学
生物
免疫学
离子通道
基因
遗传学
受体
癌症
转移
机械敏感通道
作者
Dongwon Choi,Eunkyung Park,Eunson Jung,Boksik Cha,Somin Lee,James Yu,Paul Kim,Sunju Lee,Yeo Jin Hong,Chester J. Koh,Chang-Won Cho,Yifan Wu,Noo Li Jeon,Alex K. Wong,Laura Shin,S. Ram Kumar,Iván Bermejo-Moreno,R. Sathish Srinivasan,Il-Taeg Cho,Young-Kwon Hong
出处
期刊:JCI insight
[American Society for Clinical Investigation]
日期:2019-01-24
卷期号:4 (5)
被引量:129
标识
DOI:10.1172/jci.insight.125068
摘要
The lymphatic system plays crucial roles in tissue homeostasis, lipid absorption, and immune cell trafficking. Although lymphatic valves ensure unidirectional lymph flows, the flow itself controls lymphatic valve formation. Here, we demonstrate that a mechanically activated ion channel Piezo1 senses oscillating shear stress (OSS) and incorporates the signal into the genetic program controlling lymphatic valve development and maintenance. Time-controlled deletion of Piezo1 using a pan-endothelial Cre driver (Cdh5[PAC]-CreERT2) or lymphatic-specific Cre driver (Prox1-CreERT2) equally inhibited lymphatic valve formation in newborn mice. Furthermore, Piezo1 deletion in adult lymphatics caused substantial lymphatic valve degeneration. Piezo1 knockdown in cultured lymphatic endothelial cells (LECs) largely abrogated the OSS-induced upregulation of the lymphatic valve signature genes. Conversely, ectopic Piezo1 overexpression upregulated the lymphatic valve genes in the absence of OSS. Remarkably, activation of Piezo1 using chemical agonist Yoda1 not only accelerated lymphatic valve formation in animals, but also triggered upregulation of some lymphatic valve genes in cultured LECs without exposure to OSS. In summary, our studies together demonstrate that Piezo1 is the force sensor in the mechanotransduction pathway controlling lymphatic valve development and maintenance, and Piezo1 activation is a potentially novel therapeutic strategy for congenital and surgery-associated lymphedema.
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