| Literature DB >> 33862151 |
Roberto Coppo1, Francesca Orso1, Federico Virga2, Alberto Dalmasso1, Desirée Baruffaldi1, Lei Nie3, Fabiana Clapero4, Daniela Dettori1, Lorena Quirico1, Elena Grassi1, Paola Defilippi1, Paolo Provero5, Donatella Valdembri6, Guido Serini6, Mehran M Sadeghi3, Massimiliano Mazzone2, Daniela Taverna7.
Abstract
An interactive crosstalk between tumor and stroma cells is essential for metastatic melanoma progression. We evidenced that ESDN/DCBLD2/CLCP1 plays a crucial role in endothelial cells during the spread of melanoma. Precisely, increased extravasation and metastasis formation were revealed in ESDN-null mice injected with melanoma cells, even if the primary tumor growth, vessel permeability, and angiogenesis were not enhanced. Interestingly, improved adhesion of melanoma cells to ESDN-depleted endothelial cells was observed, due to the presence of higher levels of E-selectin transcripts/proteins in ESDN-defective cells. In accordance with these results, anticorrelation was observed between ESDN and E-selectin in human endothelial cells. Most importantly, our data revealed that cimetidine, an E-selectin inhibitor, was able to block cell adhesion, extravasation, and metastasis formation in ESDN-null mice, underlying a major role of ESDN in E-selectin transcription upregulation, which according to our data, may presumably be linked to STAT3. Based on our results, we propose a protective role for ESDN during the spread of melanoma and reveal its therapeutic potential.Entities:
Keywords: Adhesion; Cimetidine; ESDN; Melanoma metastasis; Tumor microenvironment
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Year: 2021 PMID: 33862151 PMCID: PMC8581997 DOI: 10.1016/j.canlet.2021.04.005
Source DB: PubMed Journal: Cancer Lett ISSN: 0304-3835 Impact factor: 9.756