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Plexin-B3 expression stimulates MET signaling, breast cancer stem cell specification, and lung metastasis

Qiaozhu Zuo, Yongkang Yang, Yajing Lyu, Chen Yang, Chelsey Chen, Shaima Salman, Tina Yi-Ting Huang, Elizabeth E. Wicks, Walter Jackson, Emmanuel Datan, Wenxin Qin, Gregg L. Semenza

2023Cell Reports14 citationsDOIOpen Access PDF

Abstract

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.

Topics & Concepts

MetastasisBreast cancerStem cellCancer researchCancer stem cellBiologyPlexinBreast cancer metastasisSignal transductionInternal medicineOncologyCancerMedicineCell biologyCancer metastasisReceptorSemaphorinAxon Guidance and Neuronal SignalingCancer Cells and MetastasisNeonatal Respiratory Health Research
Plexin-B3 expression stimulates MET signaling, breast cancer stem cell specification, and lung metastasis | Litcius