ABSTRACT Tumor‐derived exosomes critically mediate metastasis, yet how specific cargoes reprogram the vasculature remains unclear. In gastric cancer (GC), we identify TAGLN2 as a key exosomal mediator. It is co‐overexpressed in GC cells and tumor‐associated endothelial cells (TECs), and its high endothelial expression correlates with lymph node metastasis and poor prognosis. Functionally, GC‐derived exosomes deliver TAGLN2 to endothelial cells (ECs), orchestrating angiogenesis, EndoMT, and the disruption of endothelial junctions. In vivo, exosomal TAGLN2 accelerated tumor growth and lung metastasis by generating abnormal, leaky vasculature and hypoxia. Mechanistically, exosomal TAGLN2 initiates a novel signaling axis: it transcriptionally upregulates NRP1 via c‐Jun/SP1 and concurrently induces SEMA4D expression. TAGLN2 then interacts with both NRP1 and SEMA4D to nucleate a stable cytoplasmic ternary complex. This complex dually activates YAP by competitively disrupting NRP1‐YAP binding to release YAP from cytoplasmic retention, and simultaneously suppressing Hippo‐mediated degradation, operating independently of the canonical SEMA4D‐PlexinB1‐RhoA/ROCK pathway. Therapeutically, targeting the TAGLN2 axis synergized with both cisplatin and bevacizumab, potently suppressing tumor progression by impairing neovascularization and promoting vascular normalization. Clinically, exosomal TAGLN2 levels were significantly elevated in GC patient serum. Our study delineates a complete exosome‐to‐vasculature signaling axis and positions TAGLN2/NRP1/SEMA4D/YAP module as an integrated diagnostic and therapeutic target against metastatic GC.
Yu et al. (Fri,) studied this question.