Literature DB >> 25146643

Modeling astrocytoma pathogenesis in vitro and in vivo using cortical astrocytes or neural stem cells from conditional, genetically engineered mice.

Robert S McNeill1, Ralf S Schmid2, Ryan E Bash3, Mark Vitucci4, Kristen K White1, Andrea M Werneke3, Brian H Constance5, Byron Huff6, C Ryan Miller7.   

Abstract

Current astrocytoma models are limited in their ability to define the roles of oncogenic mutations in specific brain cell types during disease pathogenesis and their utility for preclinical drug development. In order to design a better model system for these applications, phenotypically wild-type cortical astrocytes and neural stem cells (NSC) from conditional, genetically engineered mice (GEM) that harbor various combinations of floxed oncogenic alleles were harvested and grown in culture. Genetic recombination was induced in vitro using adenoviral Cre-mediated recombination, resulting in expression of mutated oncogenes and deletion of tumor suppressor genes. The phenotypic consequences of these mutations were defined by measuring proliferation, transformation, and drug response in vitro. Orthotopic allograft models, whereby transformed cells are stereotactically injected into the brains of immune-competent, syngeneic littermates, were developed to define the role of oncogenic mutations and cell type on tumorigenesis in vivo. Unlike most established human glioblastoma cell line xenografts, injection of transformed GEM-derived cortical astrocytes into the brains of immune-competent littermates produced astrocytomas, including the most aggressive subtype, glioblastoma, that recapitulated the histopathological hallmarks of human astrocytomas, including diffuse invasion of normal brain parenchyma. Bioluminescence imaging of orthotopic allografts from transformed astrocytes engineered to express luciferase was utilized to monitor in vivo tumor growth over time. Thus, astrocytoma models using astrocytes and NSC harvested from GEM with conditional oncogenic alleles provide an integrated system to study the genetics and cell biology of astrocytoma pathogenesis in vitro and in vivo and may be useful in preclinical drug development for these devastating diseases.

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Year:  2014        PMID: 25146643      PMCID: PMC4827968          DOI: 10.3791/51763

Source DB:  PubMed          Journal:  J Vis Exp        ISSN: 1940-087X            Impact factor:   1.355


  54 in total

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Journal:  J Vis Exp       Date:  2011-01-11       Impact factor: 1.355

7.  Cooperativity within and among Pten, p53, and Rb pathways induces high-grade astrocytoma in adult brain.

Authors:  Lionel M L Chow; Raelene Endersby; Xiaoyan Zhu; Sherri Rankin; Chunxu Qu; Junyuan Zhang; Alberto Broniscer; David W Ellison; Suzanne J Baker
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8.  Genetically engineered models have advantages over xenografts for preclinical studies.

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Review 10.  Genetically engineered mouse models of brain cancer and the promise of preclinical testing.

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Journal:  Brain Pathol       Date:  2009-01       Impact factor: 6.508

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Review 3.  Contemporary murine models in preclinical astrocytoma drug development.

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4.  Intrinsic Astrocyte Heterogeneity Influences Tumor Growth in Glioma Mouse Models.

Authors:  David M Irvin; Robert S McNeill; Ryan E Bash; C Ryan Miller
Journal:  Brain Pathol       Date:  2016-04-13       Impact factor: 6.508

5.  Core pathway mutations induce de-differentiation of murine astrocytes into glioblastoma stem cells that are sensitive to radiation but resistant to temozolomide.

Authors:  Ralf S Schmid; Jeremy M Simon; Mark Vitucci; Robert S McNeill; Ryan E Bash; Andrea M Werneke; Lauren Huey; Kristen K White; Matthew G Ewend; Jing Wu; C Ryan Miller
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6.  Genomic profiles of low-grade murine gliomas evolve during progression to glioblastoma.

Authors:  Mark Vitucci; David M Irvin; Robert S McNeill; Ralf S Schmid; Jeremy M Simon; Harshil D Dhruv; Marni B Siegel; Andrea M Werneke; Ryan E Bash; Seungchan Kim; Michael E Berens; C Ryan Miller
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7.  PIK3CA missense mutations promote glioblastoma pathogenesis, but do not enhance targeted PI3K inhibition.

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8.  SNHG17 drives malignant behaviors in astrocytoma by targeting miR-876-5p/ERLIN2 axis.

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9.  Combination therapy with potent PI3K and MAPK inhibitors overcomes adaptive kinome resistance to single agents in preclinical models of glioblastoma.

Authors:  Robert S McNeill; Demitra A Canoutas; Timothy J Stuhlmiller; Harshil D Dhruv; David M Irvin; Ryan E Bash; Steven P Angus; Laura E Herring; Jeremy M Simon; Kasey R Skinner; Juanita C Limas; Xin Chen; Ralf S Schmid; Marni B Siegel; Amanda E D Van Swearingen; Michael J Hadler; Erik P Sulman; Jann N Sarkaria; Carey K Anders; Lee M Graves; Michael E Berens; Gary L Johnson; C Ryan Miller
Journal:  Neuro Oncol       Date:  2017-10-19       Impact factor: 12.300

  9 in total

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