| Literature DB >> 28288873 |
Krzysztof Klimkiewicz1, Kazimierz Weglarczyk2, Guillaume Collet2, Maria Paprocka3, Alan Guichard2, Michal Sarna4, Alicja Jozkowicz5, Jozef Dulak6, Tadeusz Sarna4, Catherine Grillon2, Claudine Kieda7.
Abstract
Tumour microenvironment determines the fate of treatments. Reconstitution of tumour conditions is mandatory for alternative in vitro methods devoted to cancer development and the selection of therapeutic strategies. This work describes a 3D model of melanoma growth in its environment. Introducing means to mimic tumour angiogenesis, which turns on tumour progression, the model shows that melanoma tumour spheroids allow reconstitution of solid tumours with stromal cells. Angiogenesis evidenced the differential recruitment of endothelial cells (EC) from early progenitors (EEPCs) to mature ECs. Hypoxia was the key parameter that selected and stabilized melanoma cancer stem like cells (CSCs) phenotype based on aldehyde dehydrogenase expression as the best criterion. The 3D-tumour-model demonstrated the distinct reactivity of ECs toward tumour cells in terms of cellular cross-talk and humoral response. Intra-spheroid cell-to-cell membrane dye exchanges, mediated by intercellular interactions, uncovered the melanoma-to-EEPC cooperation. The resulting changes in tumour milieu were evidenced by the chemokinic composition and hypoxia-related variations in microRNA expression assessed in each cellular component of the spheroids. This method brings new tools to decipher the molecular mechanism of tumour-mediated cell recruitment and for in vitro assessment of therapeutic approaches.Entities:
Keywords: Angiogenesis; Endothelial progenitors; Hypoxia; Recruitment; Spheroid tumour model; microRNA
Mesh:
Year: 2017 PMID: 28288873 DOI: 10.1016/j.canlet.2017.03.006
Source DB: PubMed Journal: Cancer Lett ISSN: 0304-3835 Impact factor: 8.679