Quantitative phosphoproteomic analysis of the STAT3/IL-6/HIF1alpha signaling network: an initial study in GSC11 glioblastoma stem cells

Forskningsoutput: TidskriftsbidragArtikel i vetenskaplig tidskrift


Initiation and maintenance of several cancers including glioblastoma (GBM) may be driven by a small subset of cells called cancer stem cells (CSCs). CSCs may provide a repository of cells in tumor cell populations that are refractory to chemotherapeutic agents developed for the treatment of tumors. STAT3 is a key transcription factor associated with regulation of multiple stem cell types. Recently, a novel autocrine loop (IL-6/STAT3/HIF1alpha) has been observed in multiple tumor types (pancreatic, prostate, lung, and colon). The objective of this study was to probe perturbations of this loop in a glioblastoma cancer stem cell line (GSC11) derived from a human tumor by use of a JAK2/STAT3 phosphorylation inhibitor (WP1193), IL-6 stimulation, and hypoxia. A quantitative phosphoproteomic approach that employed phosphoprotein enrichment, chemical tagging with isobaric tags, phosphopeptide enrichment, and tandem mass spectrometry in a high-resolution instrument was applied. A total of 3414 proteins were identified in this study. A rapid Western blotting technique (<1 h) was used to confirm alterations in key protein expression and phosphorylation levels observed in the mass spectrometric experiments. About 10% of the phosphoproteins were linked to the IL-6 pathway, and the majority of remaining proteins could be assigned to other interlinked networks. By multiple comparisons between the sample conditions, we observed expected changes and gained novel insights into the contribution of each factor to the IL6/STAT3/HIF1alpha autocrine loop and the CSC response to perturbations by hypoxia, inhibition of STAT3 phosphorylation, and IL-6 stimulation.


  • Carol L Nilsson
  • Roslyn Dillon
  • Arugadoss Devakumar
  • Stone D-H Shi
  • Michael J Greig
  • John C Rogers
  • Bryan Krastins
  • Michael Rosenblatt
  • Gregory Kilmer
  • Michael Major
  • Barbara J Kaboord
  • David Sarracino
  • Taha Rezai
  • Amol Prakash
  • Mary Lopez
  • Yongjie Ji
  • Waldemar Priebe
  • Frederick Lang
  • Howard Colman
  • Charles A. Conrad
Externa organisationer
  • Pfizer


Sidor (från-till)430-443
Antal sidor14
TidskriftJournal of Proteome Research
StatusPublished - 2010 jan
Peer review utfördJa
Externt publiceradJa