BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Prostate, Early pregnancy factor, Doxorubicin, rs4950928, BRCA1, cell-cell adhesion)
Bookmark Forward

Oncogenic Mutations in Armadillo Repeats 5 and 6 of β-Catenin Reduce Binding to APC, Increasing Signaling and Transcription of Target Genes.

Pengyu Liu, Binyong Liang, Menggang Liu, Joyce H G Lebbink, Shan Li, Manning Qian, Marla Lavrijsen, Maikel P Peppelenbosch, Xin Chen, Ron Smits

Gastroenterology 2020 Mar


filter terms:
  • amino acid (2)
  • APC (3)
  • apc genes (1)
  • armadillo (3)
  • AXIN1 (1)
  • BTRC (1)
  • cancer (2)
  • ctnnb1 protein, human (1)
  • factors (1)
  • genes (2)
  • GSK3 (1)
  • half life (1)
  • humans (1)
  • immunoblots (1)
  • impair (1)
  • liver (2)
  • liver tumors (4)
  • mice (6)
  • plasmids (4)
  • promotes tumors (1)
  • protein human (1)
  • target genes (1)
  • TCF (1)
  • TCF7L2 (1)
  • Wnt (1)
  • β Catenin (19)
    • Sizes of these terms reflect their relevance to your search.

    The β-catenin signaling pathway is one of the most commonly deregulated pathways in cancer cells. Amino acid substitutions within armadillo repeats 5 and 6 (K335, W383, and N387) of β-catenin are found in several tumor types, including liver tumors. We investigated the mechanisms by which these substitutions increase signaling and the effects on liver carcinogenesis in mice. Plasmids encoding tagged full-length β-catenin (CTNNB1) or β-catenin with the K335I or N387K substitutions, along with MET, were injected into tails of FVB/N mice. Tumor growth was monitored, and livers were collected and analyzed by histology, immunohistochemistry, and quantitative reverse-transcription polymerase chain reaction. Tagged full-length and mutant forms of β-catenin were expressed in HEK293, HCT116, and SNU449 cells, which were analyzed by immunoblots and immunoprecipitation. A panel of β-catenin variants and cell lines with knock-in mutations were analyzed for differences in N-terminal phosphorylation, half-life, and association with other proteins in the signaling pathway. Mice injected with plasmids encoding K335I or N387K β-catenin and MET developed larger, more advanced tumors than mice injected with plasmids encoding WT β-catenin and MET. K335I and N387K β-catenin bound APC with lower affinity than WT β-catenin but still interacted with scaffold protein AXIN1 and in the nucleus with TCF7L2. This interaction resulted in increased transcription of genes regulated by β-catenin. Studies of protein structures supported the observed changes in relative binding affinities. Expression of β-catenin with mutations in armadillo repeats 5 and 6, along with MET, promotes formation of liver tumors in mice. In contrast to N-terminal mutations in β-catenin that directly impair its phosphorylation by GSK3 or binding to BTRC, the K335I or N387K substitutions increase signaling via reduced binding to APC. However, these mutant forms of β-catenin still interact with the TCF family of transcription factors in the nucleus. These findings show how these amino acid substitutions increase β-catenin signaling in cancer cells. Copyright © 2020 AGA Institute. Published by Elsevier Inc. All rights reserved.

    Citation

    Pengyu Liu, Binyong Liang, Menggang Liu, Joyce H G Lebbink, Shan Li, Manning Qian, Marla Lavrijsen, Maikel P Peppelenbosch, Xin Chen, Ron Smits. Oncogenic Mutations in Armadillo Repeats 5 and 6 of β-Catenin Reduce Binding to APC, Increasing Signaling and Transcription of Target Genes. Gastroenterology. 2020 Mar;158(4):1029-1043.e10

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 31857074

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.