| Literature DB >> 27000989 |
Noémie Braekeveldt1, Caroline Wigerup1, Irene Tadeo2, Siv Beckman1, Caroline Sandén3, Jimmie Jönsson3, Jonas S Erjefält3, Ana P Berbegall2, Anna Börjesson4, Torbjörn Backman4, Ingrid Øra5, Samuel Navarro2, Rosa Noguera2, David Gisselsson6, Sven Påhlman1, Daniel Bexell7.
Abstract
Treatment of high-risk childhood neuroblastoma is a clinical challenge which has been hampered by a lack of reliable neuroblastoma mouse models for preclinical drug testing. We have previously established invasive and metastasising patient-derived orthotopic xenografts (PDXs) from high-risk neuroblastomas that retained the genotypes and phenotypes of patient tumours. Given the important role of the tumour microenvironment in tumour progression, metastasis, and treatment responses, here we analysed the tumour microenvironment of five neuroblastoma PDXs in detail. The PDXs resembled their parent tumours and retained important stromal hallmarks of aggressive lesions including rich blood and lymphatic vascularisation, pericyte coverage, high numbers of cancer-associated fibroblasts, tumour-associated macrophages, and extracellular matrix components. Patient-derived tumour endothelial cells occasionally formed blood vessels in PDXs; however, tumour stroma was, overall, of murine origin. Lymphoid cells and lymphatic endothelial cells were found in athymic nude mice but not in NSG mice; thus, the choice of mouse strain dictates tumour microenvironmental components. The murine tumour microenvironment of orthotopic neuroblastoma PDXs reflects important hallmarks of aggressive and metastatic clinical neuroblastomas. Neuroblastoma PDXs are clinically relevant models for preclinical drug testing.Entities:
Keywords: Metastasis; Neuroblastoma; Paediatric cancer; Patient-derived xenograft (PDX); Tumour microenvironment; Tumour stroma
Mesh:
Year: 2016 PMID: 27000989 DOI: 10.1016/j.canlet.2016.02.046
Source DB: PubMed Journal: Cancer Lett ISSN: 0304-3835 Impact factor: 8.679