Soluble E-cadherin promotes tumor angiogenesis and localizes to exosome surface.
Maggie K S TangPatrick Y K YuePhilip Pun-Ching IpRui-Lan HuangHung-Cheng LaiAnnie N Y CheungKa Yu TseHextan Y S NganAlice S T WongPublished in: Nature communications (2018)
The limitations of current anti-angiogenic therapies necessitate other targets with complimentary mechanisms. Here, we show for the first time that soluble E-cadherin (sE-cad) (an 80-kDa soluble form), which is highly expressed in the malignant ascites of ovarian cancer patients, is a potent inducer of angiogenesis. In addition to ectodomain shedding, we provide further evidence that sE-cad is abundantly released in the form of exosomes. Mechanistically, sE-cad-positive exosomes heterodimerize with VE-cadherin on endothelial cells and transduce a novel sequential activation of β-catenin and NFκB signaling. In vivo and clinical data prove the relevance of sE-cad-positive exosomes for malignant ascites formation and widespread peritoneal dissemination. These data advance our understanding of the molecular regulation of angiogenesis in ovarian cancer and support the therapeutic potential of targeting sE-cad. The exosomal release of sE-cad, which represents a common route for externalization in ovarian cancer, could potentially be biomarkers for diagnosis and prognosis.
Keyphrases
- coronary artery disease
- endothelial cells
- mesenchymal stem cells
- stem cells
- vascular endothelial growth factor
- electronic health record
- high glucose
- big data
- signaling pathway
- cell free
- oxidative stress
- cell proliferation
- epithelial mesenchymal transition
- wound healing
- lps induced
- pi k akt
- cancer therapy
- data analysis
- cell migration