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Home › Dataset Library › Tag: Cytoskeleton › Transcription profiling of human T-ALL cell lines treated with DMSO or SAHM1

Dataset: Transcription profiling of human T-ALL cell lines treated with DMSO or SAHM1

NOTCH proteins regulate signaling pathways involved in cellular differentiation, proliferation and death. Overactive Notch signaling as...

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NOTCH proteins regulate signaling pathways involved in cellular differentiation, proliferation and death. Overactive Notch signaling as been observed in numerous cancers and has been extensively studied in the context of T-cell acute lymphoblastic leukemia (T-ALL) where more than 50% of pateints harbour mutant NOTCH1. Small molecule modulators of these proteins would be important for understanding the role of NOTCH proteins in malignant and normal biological processes. We were interested to measure the global changes in gene expression upon treatment of the human T-ALL cell lines HPB-ALL and KOPT-K1 with either vehicle alone (DMSO) or SAHM1, an alpha-helical hydrocarbon stapled peptide derived from the MAML1 co-activator protein. Experiment Overall Design: Triplicate cultures of KOPT-K1 or HPB-ALL cells were treated with either DMSO alone or SAHM1 (20 uM) for 24 hours. Total RNA was extracted and hybridized to Affymetrix human U133 plus 2.0 microarrays (three arrays per treatment per cell line for a total of 12 arrays).

Species:
human

Samples:
12

Source:
E-GEOD-18198

Updated:
Dec.12, 2014

Registered:
Sep.15, 2014


Factors: (via ArrayExpress)
Sample
GSE18198GSM455115
GSE18198GSM455116
GSE18198GSM455117
GSE18198GSM455118
GSE18198GSM455119
GSE18198GSM455120
GSE18198GSM455121
GSE18198GSM455122
GSE18198GSM455123
GSE18198GSM455124
GSE18198GSM455125
GSE18198GSM455126

Tags

  • acute lymphoblastic leukemia
  • cell
  • leukemia
  • line
  • lymphoblastic leukemia
  • notch
  • protein

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