4.6 Article

Allelic expression imbalance of PIK3CA mutations is frequent in breast cancer and prognostically significant

Journal

NPJ BREAST CANCER
Volume 8, Issue 1, Pages -

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s41523-022-00435-9

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Categories

Funding

  1. FCT-FundacAo para a Ciencia e a Tecnologia [ALG-01-0145-FEDER-31477, ALG-01-0145-FEDER-30895, CBMR-UID/BIM/04773/2013, UIDB/4255/2020, POCI-01-0145-FEDER-022184, DL 57/2016/CP1361/CT0042, SFRH/BPD/99502/2014, PD/BD/114252/2016]
  2. European Union [303745]
  3. Maratona da Saude Award
  4. Cancer Research UK
  5. British Columbia Cancer Foundation
  6. Canadian Breast Cancer Foundation BC/Yukon
  7. CRUK [C507/A16278, A16942]
  8. University of Cambridge, Hutchinson Whampoa
  9. NIHR Cambridge Biomedical Research Centre
  10. Cambridge Experimental Cancer Medicine Centre
  11. Centre for Translational Genomics (CTAG) Vancouver
  12. BCCA Breast Cancer Outcomes Unit
  13. National Institute for Health Research Cambridge Biomedical Research Centre
  14. Fundação para a Ciência e a Tecnologia [DL 57/2016/CP1361/CT0042, PD/BD/114252/2016] Funding Source: FCT

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PIK3CA mutations are common in breast cancer, and there is an allelic expression imbalance between the mutant and wild-type alleles. Preferential expression of the mutant allele is associated with poor prognosis, and ER-, PR-, and HER2+ tumors show significant preferential expression of the mutant allele.
PIK3CA mutations are the most common in breast cancer, particularly in the estrogen receptor-positive cohort, but the benefit of PI3K inhibitors has had limited success compared with approaches targeting other less common mutations. We found a frequent allelic expression imbalance between the missense mutant and wild-type PIK3CA alleles in breast tumors from the METABRIC (70.2%) and the TCGA (60.1%) projects. When considering the mechanisms controlling allelic expression, 27.7% and 11.8% of tumors showed imbalance due to regulatory variants in cis, in the two studies respectively. Furthermore, preferential expression of the mutant allele due to cis-regulatory variation is associated with poor prognosis in the METABRIC tumors (P = 0.031). Interestingly, ER-, PR-, and HER2+ tumors showed significant preferential expression of the mutated allele in both datasets. Our work provides compelling evidence to support the clinical utility of PIK3CA allelic expression in breast cancer in identifying patients of poorer prognosis, and those with low expression of the mutated allele, who will unlikely benefit from PI3K inhibitors. Furthermore, our work proposes a model of differential regulation of a critical cancer-promoting gene in breast cancer.

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