4.8 Article

The ErbB2ΔEx16 splice variant is a major oncogenic driver in breast cancer that promotes a pro-metastatic tumor microenvironment

Journal

ONCOGENE
Volume 35, Issue 47, Pages 6053-6064

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/onc.2016.129

Keywords

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Funding

  1. Terry Fox Foundation [020002]
  2. Canadian Institutes of Health Research [MOP 93525, MOP 89751]
  3. National Institutes of Health [PO1 (2PO1CA099031-06A1)]
  4. CRC Chair in Molecular Oncology
  5. Department of Defense Breast Cancer Predoctoral Traineeship [W81XWH 10-1-0114]
  6. Susan G Komen Breast Cancer Foundation [CCR14299200]
  7. NIH-NCI [T32-CA009111]
  8. NIH [R01CA160514]
  9. US-NCI [U01 CA141582]

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Amplification and overexpression of erbB2/neu proto-oncogene is observed in 20-30% human breast cancer and is inversely correlated with the survival of the patient. Despite this, somatic activating mutations within erbB2 in human breast cancers are rare. However, we have previously reported that a splice isoform of erbB2, containing an in-frame deletion of exon 16 (herein referred to as ErbB2 Delta Ex16), results in oncogenic activation of erbB2 because of constitutive dimerization of the ErbB2 receptor. Here, we demonstrate that the ErbB2 Delta Ex16 is a major oncogenic driver in breast cancer that constitutively signals from the cell surface. We further show that inducible expression of the ErbB2 Delta Ex16 variant in mammary gland of transgenic mice results in the rapid development of metastatic multifocal mammary tumors. Genetic and biochemical characterization of the ErbB2 Delta Ex16-derived mammary tumors exhibit several unique features that distinguish this model from the conventional ErbB2 ones expressing the erbB2 proto-oncogene in mammary epithelium. Unlike the wild-type ErbB2-derived tumors that express luminal keratins, ErbB2 Delta Ex16-derived tumors exhibit high degree of intratumoral heterogeneity co-expressing both basal and luminal keratins. Consistent with these distinct pathological features, the ErbB2 Delta Ex16 tumors exhibit distinct signaling and gene expression profiles that correlate with activation of number of key transcription factors implicated in breast cancer metastasis and cancer stem cell renewal.

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