Publication | Open Access
Plexin-B3 expression stimulates MET signaling, breast cancer stem cell specification, and lung metastasis
12
Citations
38
References
2023
Year
Breast OncologyCancer BiologyTumor BiologyBreast Cancer ProgressionIntratumoral HypoxiaCancer Cell BiologyStem CellsRadiation OncologyCell SignalingCancer ResearchHealth SciencesLung MetastasisHypoxia-inducible Factor 1Cell BiologyTumor MicroenvironmentStem Cell ResearchBreast CancerTumor SuppressorMedicineCancer Growth
Intratumoral hypoxia is a microenvironmental feature that promotes breast cancer progression and is associated with cancer mortality. Plexin B3 (PLXNB3) is highly expressed in estrogen receptor-negative breast cancer, but the underlying mechanisms and consequences have not been thoroughly investigated. Here, we report that PLXNB3 expression is increased in response to hypoxia and that PLXNB3 is a direct target gene of hypoxia-inducible factor 1 (HIF-1) in human breast cancer cells. PLXNB3 expression is correlated with HIF-1α immunohistochemistry, breast cancer grade and stage, and patient mortality. Mechanistically, PLXNB3 is required for hypoxia-induced MET/SRC/focal adhesion kinase (FAK) and MET/SRC/STAT3/NANOG signaling as well as hypoxia-induced breast cancer cell migration, invasion, and cancer stem cell specification. PLXNB3 knockdown impairs tumor formation and lung metastasis in orthotopic breast cancer mouse models.
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