Exon splicing analysis of intronic variants in multigene cancer panel testing for hereditary breast/ovarian cancer

The use of multigene panel testing for patients with a predisposition to breast/ovarian cancer is increasing as the identification of variants is useful for diagnosis and disease management. We identified pathogenic and likely pathogenic (P/LP) variants of high‐and moderate‐risk genes using a 23‐gen...

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Autores principales: Ryu, Jin‐Sun, Lee, Hye‐Young, Cho, Eun Hae, Yoon, Kyong‐Ah, Kim, Min‐Kyeong, Joo, Jungnam, Lee, Eun‐Sook, Kang, Han‐Sung, Lee, Seeyoun, Lee, Dong Ock, Lim, Myong Cheol, Kong, Sun‐Young
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2020
Materias:
Genetics, Genomics, and Proteomics
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7540976/
https://www.ncbi.nlm.nih.gov/pubmed/32761968
http://dx.doi.org/10.1111/cas.14600
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author Ryu, Jin‐Sun
Lee, Hye‐Young
Cho, Eun Hae
Yoon, Kyong‐Ah
Kim, Min‐Kyeong
Joo, Jungnam
Lee, Eun‐Sook
Kang, Han‐Sung
Lee, Seeyoun
Lee, Dong Ock
Lim, Myong Cheol
Kong, Sun‐Young
author_facet Ryu, Jin‐Sun
Lee, Hye‐Young
Cho, Eun Hae
Yoon, Kyong‐Ah
Kim, Min‐Kyeong
Joo, Jungnam
Lee, Eun‐Sook
Kang, Han‐Sung
Lee, Seeyoun
Lee, Dong Ock
Lim, Myong Cheol
Kong, Sun‐Young
author_sort Ryu, Jin‐Sun
collection PubMed
description The use of multigene panel testing for patients with a predisposition to breast/ovarian cancer is increasing as the identification of variants is useful for diagnosis and disease management. We identified pathogenic and likely pathogenic (P/LP) variants of high‐and moderate‐risk genes using a 23‐gene germline cancer panel in 518 patients with hereditary breast and ovarian cancers (HBOC). The frequency of P/LP variants was 12.4% (64/518) for high‐ and moderate‐penetrant genes, namely, BRCA2 (5.6%), BRCA1 (3.3%), CHEK2 (1.2%), MUTYH (0.8%), PALB2 (0.8%), MLH1 (0.4%), ATM (0.4%), BRIP1 (0.4%), TP53 (0.2%), and PMS2 (0.2%). Five patients possessed two P/LP variants in BRCA1/2 and other genes. We also compared the results from in silico splicing predictive tools and exon splicing patterns from patient samples by analyzing RT‐PCR product sequences in six P/LP intronic variants and two intronic variants of unknown significance (VUS). Altered transcriptional fragments were detected for P/LP intronic variants in BRCA1, BRIP1, CHEK2, PARB2, and PMS2. Notably, we identified an in‐frame deletion of the BRCA1 C‐terminal (BRCT) domain by exon skipping in BRCA1 c.5152+6T>C—as known VUS—indicating a risk for HBOC. Thus, exon splicing analysis can improve the identification of veiled intronic variants that would aid decision making and determination of hereditary cancer risk.
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spelling pubmed-75409762020-10-09 Exon splicing analysis of intronic variants in multigene cancer panel testing for hereditary breast/ovarian cancer Ryu, Jin‐Sun Lee, Hye‐Young Cho, Eun Hae Yoon, Kyong‐Ah Kim, Min‐Kyeong Joo, Jungnam Lee, Eun‐Sook Kang, Han‐Sung Lee, Seeyoun Lee, Dong Ock Lim, Myong Cheol Kong, Sun‐Young Cancer Sci Genetics, Genomics, and Proteomics The use of multigene panel testing for patients with a predisposition to breast/ovarian cancer is increasing as the identification of variants is useful for diagnosis and disease management. We identified pathogenic and likely pathogenic (P/LP) variants of high‐and moderate‐risk genes using a 23‐gene germline cancer panel in 518 patients with hereditary breast and ovarian cancers (HBOC). The frequency of P/LP variants was 12.4% (64/518) for high‐ and moderate‐penetrant genes, namely, BRCA2 (5.6%), BRCA1 (3.3%), CHEK2 (1.2%), MUTYH (0.8%), PALB2 (0.8%), MLH1 (0.4%), ATM (0.4%), BRIP1 (0.4%), TP53 (0.2%), and PMS2 (0.2%). Five patients possessed two P/LP variants in BRCA1/2 and other genes. We also compared the results from in silico splicing predictive tools and exon splicing patterns from patient samples by analyzing RT‐PCR product sequences in six P/LP intronic variants and two intronic variants of unknown significance (VUS). Altered transcriptional fragments were detected for P/LP intronic variants in BRCA1, BRIP1, CHEK2, PARB2, and PMS2. Notably, we identified an in‐frame deletion of the BRCA1 C‐terminal (BRCT) domain by exon skipping in BRCA1 c.5152+6T>C—as known VUS—indicating a risk for HBOC. Thus, exon splicing analysis can improve the identification of veiled intronic variants that would aid decision making and determination of hereditary cancer risk. John Wiley and Sons Inc. 2020-09-02 2020-10 /pmc/articles/PMC7540976/ /pubmed/32761968 http://dx.doi.org/10.1111/cas.14600 Text en © 2020 The Authors. Cancer Science published by John Wiley & Sons Australia, Ltd on behalf of Japanese Cancer Association. This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited and is not used for commercial purposes.
spellingShingle Genetics, Genomics, and Proteomics
Ryu, Jin‐Sun
Lee, Hye‐Young
Cho, Eun Hae
Yoon, Kyong‐Ah
Kim, Min‐Kyeong
Joo, Jungnam
Lee, Eun‐Sook
Kang, Han‐Sung
Lee, Seeyoun
Lee, Dong Ock
Lim, Myong Cheol
Kong, Sun‐Young
Exon splicing analysis of intronic variants in multigene cancer panel testing for hereditary breast/ovarian cancer
title Exon splicing analysis of intronic variants in multigene cancer panel testing for hereditary breast/ovarian cancer
title_full Exon splicing analysis of intronic variants in multigene cancer panel testing for hereditary breast/ovarian cancer
title_fullStr Exon splicing analysis of intronic variants in multigene cancer panel testing for hereditary breast/ovarian cancer
title_full_unstemmed Exon splicing analysis of intronic variants in multigene cancer panel testing for hereditary breast/ovarian cancer
title_short Exon splicing analysis of intronic variants in multigene cancer panel testing for hereditary breast/ovarian cancer
title_sort exon splicing analysis of intronic variants in multigene cancer panel testing for hereditary breast/ovarian cancer
topic Genetics, Genomics, and Proteomics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7540976/
https://www.ncbi.nlm.nih.gov/pubmed/32761968
http://dx.doi.org/10.1111/cas.14600
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