Functional analysis of clinical BARD1 germline variants
Germline pathogenic variants in BRCA1/2 account for one-third of familial breast cancers. The majority of BRCA1 function requires heterodimerization with BARD1. In contrast to BRCA1, BARD1 is a low-penetrance gene with an unclear clinical relevance, partly because of limited functional evidence. Usi...
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sg-ntu-dr.10356-1441792020-11-01T05:16:47Z Functional analysis of clinical BARD1 germline variants Toh, Ming Ren Chong, Siao Ting Chan, Sock Hoai Low, Chen Ee Nur Diana Binte Ishak Lim, Jing Quan Courtney, Eliza Ngeow, Joanne Lee Kong Chian School of Medicine (LKCMedicine) Institute of Molecular and Cellular Biology, A*STAR Science::Medicine Germline Mutation BARD1 Gene Germline pathogenic variants in BRCA1/2 account for one-third of familial breast cancers. The majority of BRCA1 function requires heterodimerization with BARD1. In contrast to BRCA1, BARD1 is a low-penetrance gene with an unclear clinical relevance, partly because of limited functional evidence. Using patient-derived lymphoblastoid cells, we functionally characterized two pathogenic variants (c.1833dupT, c.2099delG) and three variants of uncertain significance (VUSs) (c.73G>C, c.1217G>A, c.1918C>A). Three of these patients had breast cancers, whereas the remaining had colorectal cancers (n = 3). Both patients with pathogenic variants (c.1833dupT, c.2099delG) developed breast cancers with aggressive disease phenotypes such as triple-negative breast cancer and high cancer grades. As BARD1 encompasses multiple functional domains, including those of apoptosis and homologous recombination repair, we hypothesized that the function being impaired would correspond with the domain where the variant was located. Variants c.1918C>A, c.1833dupT, c.1217G>A, and c.2099delG, located within and proximal to apoptotic domains of ankyrin and BRCT, were associated with impaired apoptosis. Conversely, apoptosis function was preserved in c.73G>C, which was distant from the ankyrin domain. All variants displayed normal BRCA1 heterodimerization and RAD51 colocalization, consistent with their location being distal to BRCA1-and RAD51-binding domains. In view of deficient apoptosis, VUSs (c.1217G>A and c.1918C>A) may be pathogenic or likely pathogenic variants. In summary, functional analysis of BARD1 VUSs requires a combination of assays and, more importantly, the use of appropriate functional assays with consideration to the variant's location. National Medical Research Council (NMRC) Published version We thank our sources of support: National Medical Research Council (CSA) (NMRC/CSAINV/0017/2017) and Singhealth Foundation Research Grant (SHF/PRISM002/2015) to J.N. and SingHealth (SMSTDA-Project FY2018) to M.R.T. 2020-10-19T09:22:03Z 2020-10-19T09:22:03Z 2019 Journal Article Toh, M. R., Chong, S. T., Chan, S. H., Low, C. E., Nur Diana Binte Ishak, Lim, J. Q., ... Ngeow, J. (2019). Functional analysis of clinical BARD1 germline variants. Molecular Case Studies, 5(4), a004093-. doi:10.1101/mcs.a004093 2373-2873 https://hdl.handle.net/10356/144179 10.1101/mcs.a004093 31371347 4 5 en NMRC/CSAINV/0017/2017 Cold Spring Harbor molecular case studies © 2019 Toh et al. This article is distributed under the terms of the Creative Commons Attribution-NonCommercial License, which permits reuse and redistribution, except for commercial purposes, provided that the original author and source are credited. application/pdf |
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Science::Medicine Germline Mutation BARD1 Gene Toh, Ming Ren Chong, Siao Ting Chan, Sock Hoai Low, Chen Ee Nur Diana Binte Ishak Lim, Jing Quan Courtney, Eliza Ngeow, Joanne Functional analysis of clinical BARD1 germline variants |
| description |
Germline pathogenic variants in BRCA1/2 account for one-third of familial breast cancers. The majority of BRCA1 function requires heterodimerization with BARD1. In contrast to BRCA1, BARD1 is a low-penetrance gene with an unclear clinical relevance, partly because of limited functional evidence. Using patient-derived lymphoblastoid cells, we functionally characterized two pathogenic variants (c.1833dupT, c.2099delG) and three variants of uncertain significance (VUSs) (c.73G>C, c.1217G>A, c.1918C>A). Three of these patients had breast cancers, whereas the remaining had colorectal cancers (n = 3). Both patients with pathogenic variants (c.1833dupT, c.2099delG) developed breast cancers with aggressive disease phenotypes such as triple-negative breast cancer and high cancer grades. As BARD1 encompasses multiple functional domains, including those of apoptosis and homologous recombination repair, we hypothesized that the function being impaired would correspond with the domain where the variant was located. Variants c.1918C>A, c.1833dupT, c.1217G>A, and c.2099delG, located within and proximal to apoptotic domains of ankyrin and BRCT, were associated with impaired apoptosis. Conversely, apoptosis function was preserved in c.73G>C, which was distant from the ankyrin domain. All variants displayed normal BRCA1 heterodimerization and RAD51 colocalization, consistent with their location being distal to BRCA1-and RAD51-binding domains. In view of deficient apoptosis, VUSs (c.1217G>A and c.1918C>A) may be pathogenic or likely pathogenic variants. In summary, functional analysis of BARD1 VUSs requires a combination of assays and, more importantly, the use of appropriate functional assays with consideration to the variant's location. |
| author2 |
Lee Kong Chian School of Medicine (LKCMedicine) |
| author_facet |
Lee Kong Chian School of Medicine (LKCMedicine) Toh, Ming Ren Chong, Siao Ting Chan, Sock Hoai Low, Chen Ee Nur Diana Binte Ishak Lim, Jing Quan Courtney, Eliza Ngeow, Joanne |
| format |
Article |
| author |
Toh, Ming Ren Chong, Siao Ting Chan, Sock Hoai Low, Chen Ee Nur Diana Binte Ishak Lim, Jing Quan Courtney, Eliza Ngeow, Joanne |
| author_sort |
Toh, Ming Ren |
| title |
Functional analysis of clinical BARD1 germline variants |
| title_short |
Functional analysis of clinical BARD1 germline variants |
| title_full |
Functional analysis of clinical BARD1 germline variants |
| title_fullStr |
Functional analysis of clinical BARD1 germline variants |
| title_full_unstemmed |
Functional analysis of clinical BARD1 germline variants |
| title_sort |
functional analysis of clinical bard1 germline variants |
| publishDate |
2020 |
| url |
https://hdl.handle.net/10356/144179 |
| _version_ |
1683493429975187456 |