Notch1 and Notch2 have opposite effects on embryonal brain tumor growth

Xing Fan, Irina Mikolaenko, Ihab Elhassan, XingZhi Ni, Yunyue Wang, Douglas Ball, Daniel J. Brat, Arie Perry, Charles G. Eberhart*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

350 Scopus citations

Abstract

The role of Notch signaling in tumorigenesis can vary; Notch1 acts as an oncogene in some neoplasms, and a tumor suppressor in others. Here, we show that different Notch receptors can have opposite effects in a single tumor type. Expression of truncated, constitutively active Notch1 or Notch2 in embryonal brain tumor cell lines caused antagonistic effects on tumor growth. Cell proliferation, soft agar colony formation, and xenograft growth were all promoted by Notch2 and inhibited by Notch1. We also found that Notch2 receptor transcripts are highly expressed in progenitor cell-derived brain tumors such as medulloblastomas, whereas Notch1 is scarce or undetectable. This parallels normal cerebellar development, during which Notch2 is predominantly expressed in proliferating progenitors and Notch1 in postmitotic differentiating cells. Given the oncogenic effects of Notch2, we analyzed its gene dosage in 40 embryonal brain tumors, detecting an increased copy number in 15% of cases. Notch2 gene amplification was confirmed by fluorescence in situ hybridization in one case with extremely high Notch2 mRNA levels. In addition, expression of the Notch pathway target gene Hes1 in medulloblastomas was associated with significantly shorter patient survival (P = 0.01). Finally, pharmacological inhibition of Notch signaling suppresses growth of medulloblastoma cells. Our data indicate that Notch1 and Notch2 can have opposite effects on the growth of a single tumor type, and show that Notch2 can be overexpressed after gene amplification in human tumors.

Original languageEnglish (US)
Pages (from-to)7787-7793
Number of pages7
JournalCancer Research
Volume64
Issue number21
DOIs
StatePublished - Nov 1 2004

Funding

ASJC Scopus subject areas

  • Cancer Research
  • Oncology

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