Breast Tumors Interfere with Endothelial TRAIL at the Premetastatic Niche to Promote Cancer Cell Seeding

Overview

Journal Sci Adv

Specialties Biology
Science

Date 2023 Mar 22

PMID 36947620

Authors

Carla Riera-Domingo

Eduarda Leite-Gomes

Iris Charatsidou

Peihua Zhao

Giovanna Carra

Federica Cappellesso

Larissa Mourao

Maxim De Schepper

Dana Liu

Jens Serneels

Mohamad-Gabriel Alameh

Vladimir V Shuvaev

Tatjana Geukens

Edoardo Isnaldi

Hans Prenen

Drew Weissman

Vladimir R Muzykantov

Stefaan Soenen

Christine Desmedt

Colinda L G J Scheele

Anna Sablina

Mario Di Matteo

Rosa Martin-Perez

Massimiliano Mazzone

Affiliations

Soon will be listed here.

Abstract

Endothelial cells (ECs) grant access of disseminated cancer cells to distant organs. However, the molecular players regulating the activation of quiescent ECs at the premetastatic niche (PMN) remain elusive. Here, we find that ECs at the PMN coexpress tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) and its cognate death receptor 5 (DR5). Unexpectedly, endothelial TRAIL interacts intracellularly with DR5 to prevent its signaling and preserve a quiescent vascular phenotype. In absence of endothelial TRAIL, DR5 activation induces EC death and nuclear factor κB/p38-dependent EC stickiness, compromising vascular integrity and promoting myeloid cell infiltration, breast cancer cell adhesion, and metastasis. Consistently, both down-regulation of endothelial TRAIL at the PMN by proangiogenic tumor-secreted factors and the presence of the endogenous TRAIL inhibitors decoy receptor 1 (DcR1) and DcR2 favor metastasis. This study discloses an intracrine mechanism whereby TRAIL blocks DR5 signaling in quiescent endothelia, acting as gatekeeper of the vascular barrier that is corrupted by the tumor during cancer cell dissemination.

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