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A novel L1CAM isoform with angiogenic activity generated by NOVA2-mediated alternative splicing.


ABSTRACT: The biological players involved in angiogenesis are only partially defined. Here, we report that endothelial cells (ECs) express a novel isoform of the cell-surface adhesion molecule L1CAM, termed L1-?TM. The splicing factor NOVA2, which binds directly to L1CAM pre-mRNA, is necessary and sufficient for the skipping of L1CAM transmembrane domain in ECs, leading to the release of soluble L1-?TM. The latter exerts high angiogenic function through both autocrine and paracrine activities. Mechanistically, L1-?TM-induced angiogenesis requires fibroblast growth factor receptor-1 signaling, implying a crosstalk between the two molecules. NOVA2 and L1-?TM are overexpressed in the vasculature of ovarian cancer, where L1-?TM levels correlate with tumor vascularization, supporting the involvement of NOVA2-mediated L1-?TM production in tumor angiogenesis. Finally, high NOVA2 expression is associated with poor outcome in ovarian cancer patients. Our results point to L1-?TM as a novel, EC-derived angiogenic factor which may represent a target for innovative antiangiogenic therapies.

SUBMITTER: Angiolini F 

PROVIDER: S-EPMC6398979 | biostudies-literature | 2019 Mar

REPOSITORIES: biostudies-literature

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The biological players involved in angiogenesis are only partially defined. Here, we report that endothelial cells (ECs) express a novel isoform of the cell-surface adhesion molecule L1CAM, termed L1-ΔTM. The splicing factor NOVA2, which binds directly to <i>L1CAM</i> pre-mRNA, is necessary and sufficient for the skipping of L1CAM transmembrane domain in ECs, leading to the release of soluble L1-ΔTM. The latter exerts high angiogenic function through both autocrine and paracrine activities. Mech  ...[more]

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