Time-lapse phenotyping of invasive glioma cells ex vivo reveals subtype-specific movement patterns guided by tumor core signaling

The biology of glioblastoma invasion and its mechanisms are poorly understood. We demonstrate using time-lapse microscopy that grafting of glioblastoma (GBM) tumorspheres into rodent brain slices results in experimental ex vivo tumors with invasive properties that recapitulate the invasion observed...

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Bibliographic Details
Published in:Experimental cell research 2016-12, Vol.349 (2), p.199-213
Main Authors: Fayzullin, Artem, Tuvnes, Frode A., Skjellegrind, Håvard K., Behnan, Jinan, Mughal, Awais A., Langmoen, Iver A., Vik-Mo, Einar O.
Format: Article
Language:English
Subjects:
Brain cancer
Brain Neoplasms - pathology
Cell Line, Tumor
Cell Movement - physiology
Cell Proliferation - physiology
Cellular biology
ex vivo invasion
Gene Expression Regulation, Neoplastic
Genotype & phenotype
Glioblastoma
Glioma - pathology
Humans
Neoplasm Invasiveness - genetics
Neoplasm Invasiveness - pathology
Phenotype
Signal Transduction - genetics
Signal Transduction - physiology
Time Factors
Time-lapse
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Summary:The biology of glioblastoma invasion and its mechanisms are poorly understood. We demonstrate using time-lapse microscopy that grafting of glioblastoma (GBM) tumorspheres into rodent brain slices results in experimental ex vivo tumors with invasive properties that recapitulate the invasion observed after orthotopic transplantation into the rodent brain. The migratory movements and mitotic patterns were clearly modified by signals extrinsic to the invading cells. The cells migrated away from the tumorspheres, and removal of the spheres reduced the directed invasive movement. The cell cultures contained different populations of invasive cells that had distinct morphology and invasive behavior patterns. Grafts of the most invasive GBM culture contained 91±8% cells with an invasive phenotype, characterized by small soma with a distinct leading process. Conversely, the majority of cells in less invasive GBM grafts were phenotypically heterogeneous: only 6.3±4.1% of the cells had the invasive phenotype. Grafts of highly and moderately invasive cultures had different proportions of cells that advanced into the brain slice parenchyma during the observation period: 89.2±2.2% and 23.1±6.8%, respectively. In grafts with moderately invasive properties, most of the cells (76.8±6.8%) invading the surrounding brain tissue returned to the tumor bulk or stopped centrifugal migration. Our data suggest that the invasion of individual GBM tumors can be conditioned by the prevalence of a cell fraction with particular invasive morphology and by signaling between the tumor core and invasive cells. These findings can be important for the development of new therapeutic strategies that target the invasive GBM cells. •We used time-lapse microscopy of glioblastoma cell invasion in rodent brain slices.•Observed ex vivo invasion resembled invasive pattern found in orthotopic xenografts.•Distinct invasive cell populations with characteristic morphology and invasive patterns were identified.•Invasion and mitotic pattern were clearly modified by signals extrinsic to the invading cells.•Prevalence of cells with “specialized” invasive morphology enhances total invasion.
ISSN:0014-4827
1090-2422
DOI:10.1016/j.yexcr.2016.08.001