Literature DB >> 20721749

Functional analysis of human BRCA2 variants using a mouse embryonic stem cell-based assay.

Sergey G Kuznetsov1, Suhwan Chang, Shyam K Sharan.   

Abstract

We describe here a comprehensive and reliable assay to test the functional significance of variants of unknown clinical significance (VUS) identified in the human breast cancer susceptibility gene, BRCA2. The assay is based on the ability of human BRCA2 to complement the loss of endogenous Brca2 in mouse embryonic stem cells. The procedure involves generation of a desired mutation in BRCA2 present in a bacterial artificial chromosome (BAC) and the introduction of the BAC into ES cells engineered for the assay. These ES cells have one null and one conditional allele of Brca2. First, the effect of the BRCA2 variants on the viability of ES cells is tested by Cre-mediated deletion of the conditional allele. Subsequently, variants that result in viable ES cells are examined for their effect on known functions of BRCA2 using a variety of functional assays such as sensitivity to genotoxic agents, in vivo and in vitro proliferation, effect on homologous recombination and genomic stability. The method described herein allows for the analysis of three to five sequence variants within 2-3 months. This approach can also be used for functional analysis of variants identified in other human disease genes that result in a phenotype detectable in ES cells.

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Year:  2010        PMID: 20721749      PMCID: PMC6669890          DOI: 10.1007/978-1-60761-759-4_16

Source DB:  PubMed          Journal:  Methods Mol Biol        ISSN: 1064-3745


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Review 4.  Recombineering: a powerful new tool for mouse functional genomics.

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5.  A simple two-step, 'hit and fix' method to generate subtle mutations in BACs using short denatured PCR fragments.

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Review 8.  Functional assays for BRCA1 and BRCA2.

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2.  Assessment of the Clinical Relevance of BRCA2 Missense Variants by Functional and Computational Approaches.

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3.  Epidemiological and ES cell-based functional evaluation of BRCA2 variants identified in families with breast cancer.

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4.  Acquired cross-linker resistance associated with a novel spliced BRCA2 protein variant for molecular phenotyping of BRCA2 disruption.

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  4 in total

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