| Literature DB >> 27568559 |
Leonard D Goldstein1, James Lee2, Florian Gnad3, Christiaan Klijn3, Annalisa Schaub2, Jens Reeder3, Anneleen Daemen3, Corey E Bakalarski4, Thomas Holcomb5, David S Shames5, Ryan J Hartmaier6, Juliann Chmielecki6, Somasekar Seshagiri7, Robert Gentleman3, David Stokoe8.
Abstract
The Nrf2 pathway is frequently activated in human cancers through mutations in Nrf2 or its negative regulator KEAP1. Using a cell-line-derived gene signature for Nrf2 pathway activation, we found that some tumors show high Nrf2 activity in the absence of known mutations in the pathway. An analysis of splice variants in oncogenes revealed that such tumors express abnormal transcript variants from the NFE2L2 gene (encoding Nrf2) that lack exon 2, or exons 2 and 3, and encode Nrf2 protein isoforms missing the KEAP1 interaction domain. The Nrf2 alterations result in the loss of interaction with KEAP1, Nrf2 stabilization, induction of a Nrf2 transcriptional response, and Nrf2 pathway dependence. In all analyzed cases, transcript variants were the result of heterozygous genomic microdeletions. Thus, we identify an alternative mechanism for Nrf2 pathway activation in human tumors and elucidate its functional consequences.Entities:
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Year: 2016 PMID: 27568559 DOI: 10.1016/j.celrep.2016.08.010
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423