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Published in:

01-06-2008

Characterization of the pathogenic mechanism of a novel BRCA2 variant in a Chinese family

Authors: Ava Kwong, L. P. Wong, K. Y. K. Chan, E. S. K. Ma, U. S. Khoo, J. M. Ford

Published in: Familial Cancer | Issue 2/2008

Abstract

Introduction: Germline mutations of BRCA1 and BRCA2 account for the majority of hereditary breast cancers, many of which are classified as variants of unknown significance (VUS). We report the identification of a novel BRCA2 variant (c.7806-9T > G) in a Chinese family with multiple breast cancers and document it as a pathogenic mutation. Methods: The proband in this family was diagnosed with breast cancer at age 50 with a strong family history of breast cancer. DNA and RNA were extracted from the blood of the proband and her family, and was used for BRCA gene mutation/deletion screening and RNA splicing analysis. Results: BRCA2 c.7806-9T > G was identified in the proband, which was suggestive of a variant. This change was also found in two sisters of the proband with a history of breast cancer, as well as from the proband’s maternal gastric cancer. The only sibling free of breast cancer did not carry the BRCA2 variant, thus demonstrating that the mutation segregates with the clinical phenotype in this family. RNA analysis on the proband blood sample revealed three aberrant splicing variants: c.7806_7874del, c.7806_7976del, and c.7806-8_7806-1ins. The latter causes a frameshift and creates a truncated protein, whilst the other two splicing variants resulted in shorter forms of the protein. Conclusions: The identified BRCA2 c.7806-9T > G [Genbank: DQ889340] was found to be pathogenic, based on aberrant splicing events resulting in the formation of truncated protein products. Thus, better understanding and classification of BRCA variants as neutral or disease causing has important implications for genetic counseling so that appropriate management can be given.

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Title: Characterization of the pathogenic mechanism of a novel BRCA2 variant in a Chinese family
Authors: Ava Kwong
L. P. Wong
K. Y. K. Chan
E. S. K. Ma
U. S. Khoo
J. M. Ford
Publication date: 01-06-2008
Publisher: Springer Netherlands
Published in: Familial Cancer / Issue 2/2008
Print ISSN: 1389-9600
Electronic ISSN: 1573-7292
DOI: https://doi.org/10.1007/s10689-007-9155-7

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