Pathogenicity of the BRCA1 Missense Variant M1775K is Determined by the Disruption of the BRCT Phosphopeptide-Binding Pocket: a Multi-Modal Approach

Tischkowitz, M; Hamel, N; Carvalho, M; Birrane, G; Soni, A; van Beers, E; Joosse, S; Wong, N; Novak, D

doi:10.1038/ejhg.2008.13

Title: Pathogenicity of the BRCA1 Missense Variant M1775K is Determined by the Disruption of the BRCT Phosphopeptide-Binding Pocket: a Multi-Modal Approach

Journal Article · Tue Jan 01 00:00:00 EST 2008 · European Journal of Human Genetics

DOI:https://doi.org/10.1038/ejhg.2008.13· OSTI ID:960192

Tischkowitz, M; Hamel, N; Carvalho, M; Birrane, G; Soni, A; van Beers, E; Joosse, S; Wong, N; Novak, D

A number of germ-line mutations in the BRCA1 gene confer susceptibility to breast and ovarian cancer. However, it remains difficult to determine whether many single amino-acid (missense) changes in the BRCA1 protein that are frequently detected in the clinical setting are pathologic or not. Here, we used a combination of functional, crystallographic, biophysical, molecular and evolutionary techniques, and classical genetic segregation analysis to demonstrate that the BRCA1 missense variant M1775K is pathogenic. Functional assays in yeast and mammalian cells showed that the BRCA1 BRCT domains carrying the amino-acid change M1775K displayed markedly reduced transcriptional activity, indicating that this variant represents a deleterious mutation. Importantly, the M1775K mutation disrupted the phosphopeptide-binding pocket of the BRCA1 BRCT domains, thereby inhibiting the BRCA1 interaction with the proteins BRIP1 and CtIP, which are involved in DNA damage-induced checkpoint control. These results indicate that the integrity of the BRCT phosphopeptide-binding pocket is critical for the tumor suppression function of BRCA1. Moreover, this study demonstrates that multiple lines of evidence obtained from a combination of functional, structural, molecular and evolutionary techniques, and classical genetic segregation analysis are required to confirm the pathogenicity of rare variants of disease-susceptibility genes and obtain important insights into the underlying pathogenetic mechanisms.

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Research Organization:: Brookhaven National Lab. (BNL), Upton, NY (United States). National Synchrotron Light Source

Sponsoring Organization:: Doe - Office Of Science

DOE Contract Number:: DE-AC02-98CH10886

OSTI ID:: 960192

Report Number(s):: BNL-83178-2009-JA; TRN: US201016%%1336

Journal Information:: European Journal of Human Genetics, Vol. 16

Country of Publication:: United States

Language:: English

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59 BASIC BIOLOGICAL SCIENCES
99 GENERAL AND MISCELLANEOUS//MATHEMATICS, COMPUTING, AND INFORMATION SCIENCE
DNA
FUNCTIONALS
GENES
GENETICS
MAMMARY GLANDS
MUTATIONS
NEOPLASMS
PROTEINS
SEGREGATION
YEASTS
AMINO ACIDS
national synchrotron light source

Title: Pathogenicity of the BRCA1 Missense Variant M1775K is Determined by the Disruption of the BRCT Phosphopeptide-Binding Pocket: a Multi-Modal Approach

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