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Related Experiment Video

Updated: Sep 21, 2025

Functional Assessment of BRCA1 variants using CRISPR-Mediated Base Editors
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Comprehensive evaluation and efficient classification of BRCA1 RING domain missense substitutions.

Kathleen A Clark1, Andrew Paquette2, Kayoko Tao1

  • 1Huntsman Cancer Institute at the University of Utah, Salt Lake City, UT 84112, USA.

American Journal of Human Genetics
|June 6, 2022
PubMed
Summary
This summary is machine-generated.

This study evaluated BRCA1 RING domain missense substitutions for their impact on BARD1 heterodimerization, crucial for breast and ovarian cancer risk. The findings help classify variants, improving clinical applicability for cancer susceptibility.

Keywords:
ACMG VUS classificationBRCA1Bayesian data integrationfunctional assay calibration

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Area of Science:

  • Genetics and Genomics
  • Cancer Biology
  • Molecular Diagnostics

Background:

  • BRCA1 is a critical gene for breast and ovarian cancer susceptibility.
  • Pathogenic variants in BRCA1 include protein-truncating mutations and missense substitutions.
  • Known pathogenic missense substitutions are concentrated in the RING and BRCT domains, affecting protein function.

Purpose of the Study:

  • To systematically assess the pathogenicity of all possible BRCA1 RING domain missense substitutions.
  • To evaluate the functional impact of these substitutions on BARD1 heterodimerization.
  • To develop a clinically applicable classification system for BRCA1 missense variants.

Main Methods:

  • Utilized a mammalian two-hybrid assay to test BRCA1 RING domain missense substitutions for BARD1 heterodimerization.
  • Employed assay calibration and validation strategies.
  • Integrated functional assay data with computational predictions and human observational data using a Bayesian point system.

Main Results:

  • Identified 15%-20% of BRCA1 RING domain missense substitutions as pathogenic.
  • Achieved clinical classification for 89% of observed missense substitutions.
  • Identified additional variants with strong evidence for pathogenicity or benignity based on functional and computational data.

Conclusions:

  • Functional assessment of BRCA1 RING domain missense substitutions is vital for understanding cancer risk.
  • A combined approach integrating functional assays, computational data, and observational data enhances variant classification accuracy.
  • This framework improves the clinical interpretation of BRCA1 variants, aiding in genetic counseling and risk assessment for hereditary breast and ovarian cancer.