Senescence-induced endothelial phenotypes underpin immune-mediated senescence surveillance

Author:

Yin KelvinORCID,Patten DanielORCID,Gough Sarah,de Barros Gonçalves Susana,Chan AdelyneORCID,Olan IoanaORCID,Cassidy LiamORCID,Poblocka Marta,Zhu Haoran,Lun AaronORCID,Schuijs Martijn,Young AndrewORCID,Martinez-Jimenez CeliaORCID,Halim Timotheus Y.F.,Shetty ShishirORCID,Narita MasashiORCID,Hoare MatthewORCID

Abstract

Senescence is a stress-responsive tumor suppressor mechanism associated with expression of the senescence-associated secretory phenotype (SASP). Through the SASP, senescent cells trigger their own immune-mediated elimination, which if evaded leads to tumorigenesis. Senescent parenchymal cells are separated from circulating immunocytes by the endothelium, which is targeted by microenvironmental signaling. Here we show that SASP induces endothelial cell NF-κB activity and that SASP-induced endothelial expression of the canonical NF-κB componentRelaunderpins senescence surveillance. Using human liver sinusoidal endothelial cells (LSECs), we show that SASP-induced endothelial NF-κB activity regulates a conserved transcriptional program supporting immunocyte recruitment. Furthermore, oncogenic hepatocyte senescence drives murine LSEC NF-κB activity in vivo. Critically, we show two distinct endothelial pathways in senescence surveillance. First, endothelial-specific loss ofRelaprevents development of Stat1-expressing CD4+T lymphocytes. Second, the SASP up-regulates ICOSLG on LSECs, with the ICOS–ICOSLG axis contributing to senescence cell clearance. Our results show that the endothelium is a nonautonomous SASP target and an organizing center for immune-mediated senescence surveillance.

Funder

CRUK Advanced Clinician Scientist Fellowship

CRUK Accelerator Award

CRUK-Oregon Health and Science University

CRUK Cambridge Institute

Medical Research Council

Biotechnology and Biological Sciences Research Council

Diabetes UK

BIRAX

British Council

CRUK Pioneer

National Institute for Health and Care Research

Cambridge Biomedical Research Centre

Publisher

Cold Spring Harbor Laboratory

Subject

Developmental Biology,Genetics

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