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Literature DB >> 29185120

Characterization of a novel germline BRCA1 splice variant, c.5332+4delA.

Ciyu Yang¹, Sowmya Jairam¹, Kimberly A Amoroso², Mark E Robson², Michael F Walsh³, Liying Zhang⁴.

Abstract

PURPOSE: Germline mutations in BRCA1 and BRCA2 confer a significant increase in risk for cancer, and determining pathogenicity of a BRCA variant can guide the clinical management of the disease. About 1/3 of BRCA1 variants reported in the public databases have uncertain clinical significance due to lack of conclusive evidence. This study aims to characterize a novel BRCA1 deletion affecting the + 4 splice donor site identified in an individual with early-onset breast cancer.
METHODS: The effect of BRCA1 c.5332+4delA variant on RNA splicing was evaluated by amplifying regions of BRCA1 from cDNA derived from the patient. The proportion of abnormal transcript in the total transcripts was quantified. Loss of heterozygosity (LOH) in tumor tissue was investigated using Sanger sequencing and fragment analysis.
RESULTS: BRCA1 c.5332+4delA caused skipping of exon 21 in patient-derived samples. Semi-quantitative analysis indicated that this aberrant RT-PCR product accounts for about 40% of the total transcript levels. Loss of heterozygosity (LOH) was observed in patient's tumor tissue.
CONCLUSIONS: Our results indicate that the BRCA1 c.5332+4delA variant contributes to cancer predisposition through disruption of normal mRNA splicing. We classify this variant as likely pathogenic.

Entities: Chemical Disease Gene Mutation Species

Keywords: BRCA1; Breast cancer; Exon skipping; Germline variant; Loss of heterozygosity; Pathogenic; Splicing; c.5332+4delA

Mesh：

Substances：

Year: 2017 PMID： 29185120 PMCID： PMC6788766 DOI： 10.1007/s10549-017-4595-8

Source DB: PubMed Journal: Breast Cancer Res Treat ISSN： 0167-6806 Impact factor: 4.872

34 in total

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2. Novel bioinformatics quality control metric for next-generation sequencing experiments in the clinical context.

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Journal: NPJ Breast Cancer Date: 2022-01-17

4 in total