Endovascular progenitors infiltrate melanomas and differentiate towards a variety of vascular beds promoting tumor metastasis.
Prudence DonovanJatin PatelJames DightHo Yi WongSeen-Ling SimValentine MurigneuxMathias FrancoisKiarash KhosrotehraniPublished in: Nature communications (2019)
Tumor vascularization is a hallmark of cancer central to disease progression and metastasis. Current anti-angiogenic therapies have limited success prompting the need to better understand the cellular origin of tumor vessels. Using fate-mapping analysis of endothelial cell populations in melanoma, we report the very early infiltration of endovascular progenitors (EVP) in growing tumors. These cells harbored self-renewal and reactivated the expression of SOX18 transcription factor, initiating a vasculogenic process as single cells, progressing towards a transit amplifying stage and ultimately differentiating into more mature endothelial phenotypes that comprised arterial, venous and lymphatic subtypes within the core of the tumor. Molecular profiling by RNA sequencing of purified endothelial fractions characterized EVPs as quiescent progenitors remodeling the extracellular matrix with significant paracrine activity promoting growth. Functionally, EVPs did not rely on VEGF-A signaling whereas endothelial-specific loss of Rbpj depleted the population and strongly inhibited metastasis. The understanding of endothelial heterogeneity opens new avenues for more effective anti-vascular therapies in cancer.
Keyphrases
- endothelial cells
- transcription factor
- extracellular matrix
- induced apoptosis
- single cell
- papillary thyroid
- cell cycle arrest
- stem cells
- lymph node
- vascular endothelial growth factor
- squamous cell
- cell death
- cell proliferation
- oxidative stress
- magnetic resonance
- computed tomography
- signaling pathway
- childhood cancer
- binding protein
- genetic diversity
- neural stem cells
- pi k akt