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Home › Dataset Library › Expression data from retroviral vector-infected immortalized mouse embryonic fibroblasts (MEFs)

Dataset: Expression data from retroviral vector-infected immortalized mouse embryonic fibroblasts (MEFs)

Cultured cancer cells exhibit substantial phenotypic heterogeneity when measured in a variety of ways such as sensitivity to drugs or the...

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Cultured cancer cells exhibit substantial phenotypic heterogeneity when measured in a variety of ways such as sensitivity to drugs or the capacity to grow under various conditions. Among these, the ability to exhibit anchorage-independent cell growth (colony forming capacity in semisolid media) has been considered to be fundamental in cancer biology because it has been connected with tumor cell aggressiveness in vivo such as tumorigenic and metastatic potentials, and also utilized as a marker for in vitro transformation. Although multiple genetic factors for anchorage-independence have been identified, the molecular basis for this capacity is still largely unknown. To investigate the molecular mechanisms underlying anchorage-independent cell growth, we have used genome-wide DNA microarray studies to develop an expression signature associated with this phenotype. Using this signature, we identify a program of activated mitochondrial biogenesis associated with the phenotype of anchorage-independent growth and importantly, we demonstrate that this phenotype predicts potential for metastasis in primary breast and lung tumors. Keywords: c-Myc or v-Src retroviral vector-infected immortalized mouse embryonic fibroblasts. Expression data of c-Myc and v-Src transformed MEFs was used to validate an expression signature generated from human cultured breast cancer cell lines with anchorage-independent growth ability.

Species:
mouse

Samples:
26

Source:
E-GEOD-15161

PubMed:
19483725

Updated:
Dec.12, 2014

Registered:
Nov.11, 2014


Factors: (via ArrayExpress)
Sample VECTOR REPLICATE PARENTAL CELL LINE
GSM378662 pBabe-puro (empty vector) 1 WA
GSM378663 pBabe-puro (empty vector) 2 WA
GSM378664 pBabe-puro (empty vector) 3 WA
GSM378665 pBabe-puro (empty vector) 1 WB
GSM378666 pBabe-puro (empty vector) 2 WB
GSM378667 pBabe-puro (empty vector) 3 WB
GSM378668 pBabe-puro (empty vector) 1 WC
GSM378669 pBabe-puro (empty vector) 2 WC
GSM378670 pBabe-puro (empty vector) 3 WC
GSM37867 pBabe-human c-myc (c-myc vector) 1 WA
GSM378672 pBabe-human c-myc (c-myc vector) 2 WA
GSM378673 pBabe-human c-myc (c-myc vector) 3 WA
GSM378674 pBabe-human c-myc (c-myc vector) 1 WB
GSM378675 pBabe-human c-myc (c-myc vector) 2 WB
GSM378676 pBabe-human c-myc (c-myc vector) 3 WB
GSM378677 pBabe-human c-myc (c-myc vector) 1 WC
GSM378678 pBabe-human c-myc (c-myc vector) 2 WC
GSM378679 pBabe-human c-myc (c-myc vector) 3 WC
GSM378680 pBabe-human v-src (v-src vector) 1 WA
GSM37868 pBabe-human v-src (v-src vector) 2 WA
GSM378682 pBabe-human v-src (v-src vector) 3 WA
GSM378683 pBabe-human v-src (v-src vector) 2 WB
GSM378684 pBabe-human v-src (v-src vector) 3 WB
GSM378685 pBabe-human v-src (v-src vector) 1 WC
GSM378686 pBabe-human v-src (v-src vector) 2 WC
GSM378687 pBabe-human v-src (v-src vector) 3 WC

Tags

  • breast
  • breast cancer
  • cancer
  • cell
  • genome
  • lung
  • semisolid

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