Transcript and protein profiling identifies signaling, growth arrest, apoptosis, and NF-κB survival signatures following GNRH receptor activation

Colette Meyer, Andrew H. Sims, Kevin Morgan, Beth Harrison, Morwenna Muir, Jianing Bai, Dana Faratian, Robert P. Millar, Simon P. Langdon*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

Abstract / Description of output

GNRH significantly inhibits proliferation of a proportion of cancer cell lines by activating GNRH receptor (GNRHR)-G protein signaling. Therefore, manipulation of GNRHR signaling may have an under-utilized role in treating certain breast and ovarian cancers. However, the precise signaling pathways necessary for the effect and the features of cellular responses remain poorly defined. We used transcriptomic and proteomic profiling approaches to characterize the effects of GNRHR activation in sensitive cells (HEK293-GNRHR, SCL60) in vitro and in vivo, compared to unresponsive HEK293. Analyses of gene expression demonstrated a dynamic response to the GNRH superagonist Triptorelin. Early and midphase changes (0.5-1.0 h) comprised mainly transcription factors. Later changes (8-24 h) included a GNRH target gene, CGA, and up- or downregulation of transcripts encoding signaling and cell division machinery. Pathway analysis identified altered MAPK and cell cycle pathways, consistent with occurrence of G2/M arrest and apoptosis. Nuclear factor kappa B (NF-κB) pathway gene transcripts were differentially expressed between control and Triptorelin-treated SCL60 cultures. Reverse-phase protein and phospho-proteomic array analyses profiled responses in cultured cells and SCL60 xenografts in vivo during Triptorelin anti-proliferation. Increased phosphorylated NF-κB (p65) occurred in SCL60 in vitro, and p-NF-κB and IkB3 were higher in treated xenografts than controls after 4 days Triptorelin. NF-κB inhibition enhanced the anti-proliferative effect of Triptorelin in SCL60 cultures. This study reveals details of pathways interacting with intense GNRHR signaling, identifies potential anti-proliferative target genes, and implicates the NF-κB survival pathway as a node for enhancing GNRH agonist-induced anti-proliferation. © 2013 Society for Endocrinology.
Original languageEnglish
Pages (from-to)123-136
Number of pages14
JournalEndocrine-Related Cancer
Volume20
Issue number1
DOIs
Publication statusPublished - Feb 2013

Keywords / Materials (for Non-textual outputs)

  • NF kappa B
  • BREAST-CANCER-CELLS
  • GnRh
  • HORMONE-RELEASING HORMONE
  • HUMAN ENDOMETRIAL
  • REGULATED KINASE
  • LINES
  • ANTAGONISTS
  • xenograft
  • LNCAP
  • triptorelin
  • SCL60
  • HIGH-AFFINITY BINDING
  • EXPRESSION
  • AGONIST

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