BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. FABP1, Coagulation, Lung cancer, Intestine, Pharmacogenetics, Quercetin, rs6983267)
Bookmark Forward

Protein arginine methyltransferase 6-dependent gene expression and splicing: association with breast cancer outcomes.

Dennis H Dowhan, Matthew J Harrison, Natalie A Eriksson, Peter Bailey, Michael A Pearen, Peter J Fuller, John W Funder, Evan R Simpson, Peter J Leedman, Wayne D Tilley, Melissa A Brown, Christine L Clarke, George E O Muscat

Institute for Molecular Bioscience, The University of Queensland, Brisbane, Queensland 4072, Australia. d.dowhan@uq.edu.au

Endocrine-related cancer 2012 Aug


filter terms:
  • alternate splicing (1)
  • alternative splicing (4)
  • breast cancer (7)
  • breast tumours (4)
  • cancer (1)
  • cell cycle (1)
  • cell cycle, gene (1)
  • cell death (1)
  • cells (3)
  • cells cultured (1)
  • death cell (1)
  • endocrine function (1)
  • endocrine system development (1)
  • ESR1 (1)
  • exon (2)
  • female (1)
  • function (1)
  • gene (4)
  • gene expression (4)
  • gene expression profiling (1)
  • gene expression regulation (2)
  • gene expression regulation, enzymologic (1)
  • gene expression regulation, neoplastic (1)
  • human (3)
  • in vitro (2)
  • methyltransferases small (1)
  • microarray analysis (1)
  • normal breast (1)
  • nuclear proteins (2)
  • PRMT6 (11)
  • prmt6 protein, human (1)
  • processes (1)
  • prognosis (1)
  • protein arginine n- methyltransferases (2)
  • small interfering rna (3)
  • steroid (1)
  • transcription (3)
  • tumor cells, cultured (1)
  • tumor markers (4)
  • validation studies as topic (1)
    • Sizes of these terms reflect their relevance to your search.

    Protein arginine methyltransferase-6 (PRMT6) regulates steroid-dependent transcription and alternative splicing and is implicated in endocrine system development and function, cell death, cell cycle, gene expression and cancer. Despite its role in these processes, little is known about its function and cellular targets in breast cancer. To identify novel gene targets regulated by PRMT6 in breast cancer cells, we used a combination of small interfering RNA and exon-specific microarray profiling in vitro coupled to in vivo validation in normal breast and primary human breast tumours. This approach, which allows the examination of genome-wide changes in individual exon usage and total transcript levels, demonstrated that PRMT6 knockdown significantly affected i) the transcription of 159 genes and ii) alternate splicing of 449 genes. The PRMT6-dependent transcriptional and alternative splicing targets identified in vitro were validated in human breast tumours. Using the list of genes differentially expressed between normal and PRMT6 knockdown cells, we generated a PRMT6-dependent gene expression signature that provides an indication of PRMT6 dysfunction in breast cancer cells. Interrogation of several well-studied breast cancer microarray expression datasets with the PRMT6 gene expression signature demonstrated that PRMT6 dysfunction is associated with better overall relapse-free and distant metastasis-free survival in the oestrogen receptor (ER (ESR1)) breast cancer subgroup. These results suggest that dysregulation of PRMT6-dependent transcription and alternative splicing may be involved in breast cancer pathophysiology and the molecular consequences identifying a unique and informative biomarker profile.

    Citation

    Dennis H Dowhan, Matthew J Harrison, Natalie A Eriksson, Peter Bailey, Michael A Pearen, Peter J Fuller, John W Funder, Evan R Simpson, Peter J Leedman, Wayne D Tilley, Melissa A Brown, Christine L Clarke, George E O Muscat. Protein arginine methyltransferase 6-dependent gene expression and splicing: association with breast cancer outcomes. Endocrine-related cancer. 2012 Aug;19(4):509-26

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 22673335

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