Pathogenicity assessment of variants for breast cancer susceptibility genes based on BRCAness of tumor sample.

Szczegóły
Abstrakt

Tytuł:: Pathogenicity assessment of variants for breast cancer susceptibility genes based on BRCAness of tumor sample.
Autorzy:: Yoshida R; Department of Oncotherapeutic Medicine, Graduate School of Medicine, Tohoku University, Sendai, Japan.; Division of Cancer Genomics, Cancer Institute, Japanese Foundation for Cancer Research (JFCR), Tokyo, Japan.; Department of Clinical Genetic Oncology, Cancer Institute Hospital (CIH), JFCR, Tokyo, Japan.
Hagio T; Division of Cancer Genomics, Cancer Institute, Japanese Foundation for Cancer Research (JFCR), Tokyo, Japan.; Project for Development of Innovative Research on Cancer Therapeutics, Cancer Precision Medicine Center, JFCR, Tokyo, Japan.
Kaneyasu T; Division of Cancer Genomics, Cancer Institute, Japanese Foundation for Cancer Research (JFCR), Tokyo, Japan.; Project for Development of Innovative Research on Cancer Therapeutics, Cancer Precision Medicine Center, JFCR, Tokyo, Japan.
Gotoh O; Division of Cancer Genomics, Cancer Institute, Japanese Foundation for Cancer Research (JFCR), Tokyo, Japan.; Project for Development of Innovative Research on Cancer Therapeutics, Cancer Precision Medicine Center, JFCR, Tokyo, Japan.
Osako T; Division of Pathology, Cancer Institute, JFCR, Tokyo, Japan.
Tanaka N; Division of Cancer Genomics, Cancer Institute, Japanese Foundation for Cancer Research (JFCR), Tokyo, Japan.; Project for Development of Innovative Research on Cancer Therapeutics, Cancer Precision Medicine Center, JFCR, Tokyo, Japan.
Amino S; Division of Cancer Genomics, Cancer Institute, Japanese Foundation for Cancer Research (JFCR), Tokyo, Japan.; Project for Development of Genomics-based Cancer Medicine, Cancer Precision Medicine Center, JFCR, Tokyo, Japan.
Yaguchi N; Division of Cancer Genomics, Cancer Institute, Japanese Foundation for Cancer Research (JFCR), Tokyo, Japan.; Project for Development of Innovative Research on Cancer Therapeutics, Cancer Precision Medicine Center, JFCR, Tokyo, Japan.
Nakashima E; Breast Oncology Center, CIH, JFCR, Tokyo, Japan.
Kitagawa D; Breast Oncology Center, CIH, JFCR, Tokyo, Japan.; Department of Breast Surgical Oncology, Center Hospital of the National Center for Global Health and Medicine, Tokyo, Japan.
Ueno T; Breast Oncology Center, CIH, JFCR, Tokyo, Japan.
Ohno S; Breast Oncology Center, CIH, JFCR, Tokyo, Japan.
Nakajima T; Department of Clinical Genetic Oncology, Cancer Institute Hospital (CIH), JFCR, Tokyo, Japan.
Nakamura S; Division of Breast Surgical Oncology, Showa University School of Medicine, Tokyo, Japan.
Miki Y; Division of Genetic Diagnosis, Cancer Institute, JFCR, Tokyo, Japan.
Hirota T; Department of Cellular and Molecular Imaging of Cancer, Graduate School of Medicine, Tohoku University, Sendai, Japan.; Division of Experimental Pathology, Cancer Institute, JFCR, Tokyo, Japan.
Takahashi S; Department of Oncotherapeutic Medicine, Graduate School of Medicine, Tohoku University, Sendai, Japan.; Department of Medical Oncology, CIH, JFCR, Tokyo, Japan.
Matsuura M; Division of Cancer Genomics, Cancer Institute, Japanese Foundation for Cancer Research (JFCR), Tokyo, Japan.
Noda T; Division of Cancer Genomics, Cancer Institute, Japanese Foundation for Cancer Research (JFCR), Tokyo, Japan.; Project for Development of Genomics-based Cancer Medicine, Cancer Precision Medicine Center, JFCR, Tokyo, Japan.; Cancer, Institute, JFCR, Tokyo, Japan.
Mori S; Division of Cancer Genomics, Cancer Institute, Japanese Foundation for Cancer Research (JFCR), Tokyo, Japan.; Project for Development of Innovative Research on Cancer Therapeutics, Cancer Precision Medicine Center, JFCR, Tokyo, Japan.
Źródło:: Cancer science [Cancer Sci] 2021 Mar; Vol. 112 (3), pp. 1310-1319. Date of Electronic Publication: 2021 Feb 02.
Typ publikacji:: Journal Article; Observational Study; Validation Study
Język:: English
Imprint Name(s):: Publication: 2005- : Oxford : Wiley Publishing on behalf of the Japanese Cancer Association
Original Publication: Tokyo : Japanese Cancer Association, c2003-
MeSH Terms:: Genetic Predisposition to Disease*
Homologous Recombination*
Models, Genetic*
Biomarkers, Tumor/*genetics
Breast Neoplasms/*genetics
Adult ; Aged ; Ataxia Telangiectasia Mutated Proteins/genetics ; BRCA1 Protein/genetics ; BRCA2 Protein/genetics ; Breast/pathology ; Breast/surgery ; Breast Neoplasms/pathology ; Breast Neoplasms/surgery ; Checkpoint Kinase 2/genetics ; DNA Mutational Analysis ; Datasets as Topic ; Exome/genetics ; Fanconi Anemia Complementation Group N Protein/genetics ; Female ; Genetic Testing/methods ; Germ-Line Mutation ; Humans ; Mastectomy ; Middle Aged ; Exome Sequencing
References:: Science. 2017 Mar 17;355(6330):1152-1158. (PMID: 28302823)
Nat Commun. 2017 Aug 22;8(1):319. (PMID: 28831036)
Nat Med. 2008 Aug;14(8):875-81. (PMID: 18607349)
N Engl J Med. 2016 Dec;375(22):2154-2164. (PMID: 27717299)
Breast Cancer Res. 2015 Aug 19;17:111. (PMID: 26283626)
Cancer Res. 2008 May 1;68(9):3523-31. (PMID: 18451181)
Nature. 2020 Feb;578(7793):82-93. (PMID: 32025007)
Breast Cancer Res. 2018 Apr 17;20(1):28. (PMID: 29665859)
Int J Cancer. 2017 Apr 1;140(7):1545-1550. (PMID: 27943282)
Hum Mutat. 2009 Jan;30(1):123-33. (PMID: 18680205)
Nat Commun. 2017 Oct 11;8(1):857. (PMID: 29021619)
PLoS One. 2013;8(2):e55681. (PMID: 23409019)
Nat Med. 2017 Apr;23(4):517-525. (PMID: 28288110)
Breast Cancer Res. 2011 Oct 27;13(5):R107. (PMID: 22032731)
Lancet Oncol. 2019 May;20(5):636-648. (PMID: 30948273)
Cancer Res. 2013 Jan 1;73(1):265-75. (PMID: 23108138)
Cancer Res. 2012 Nov 1;72(21):5454-62. (PMID: 22933060)
Clin Cancer Res. 2016 Aug 1;22(15):3764-73. (PMID: 26957554)
Breast Cancer Res. 2014 Dec 05;16(6):475. (PMID: 25475740)
Nat Commun. 2018 Oct 4;9(1):4083. (PMID: 30287823)
Br J Cancer. 2012 Nov 6;107(10):1776-82. (PMID: 23047548)
Nature. 2016 May 02;534(7605):47-54. (PMID: 27135926)
Cancer Sci. 2021 Mar;112(3):1310-1319. (PMID: 33421217)
Genet Med. 2015 May;17(5):405-24. (PMID: 25741868)
Genet Med. 2018 Mar;20(3):346-350. (PMID: 29215655)
Ann Oncol. 2018 Mar 1;29(3):654-660. (PMID: 29293876)
Cancer Res. 2005 Jan 15;65(2):417-26. (PMID: 15695382)
N Engl J Med. 2015 Jun 4;372(23):2243-57. (PMID: 26014596)
Br J Cancer. 2013 May 28;108(10):2172-7. (PMID: 23558900)
Eur J Hum Genet. 2014 Nov;22(11):1305-13. (PMID: 24549055)
Nature. 2018 Oct;562(7726):217-222. (PMID: 30209399)
Cancer Discov. 2012 Apr;2(4):366-375. (PMID: 22576213)
Nat Rev Cancer. 2004 Oct;4(10):814-9. (PMID: 15510162)
Mol Cell Oncol. 2014 Jul;1(1):. (PMID: 26203462)
Nature. 2013 Aug 22;500(7463):415-21. (PMID: 23945592)
Nat Genet. 2017 Oct;49(10):1476-1486. (PMID: 28825726)
Nat Rev Cancer. 2016 Feb;16(2):110-20. (PMID: 26775620)
NPJ Breast Cancer. 2020 Jun 12;6:25. (PMID: 32566746)
Elife. 2017 Apr 11;6:. (PMID: 28398198)
Cancer Epidemiol Biomarkers Prev. 2012 Jan;21(1):134-47. (PMID: 22144499)
J Law Biosci. 2018 Jan 22;4(3):648-657. (PMID: 29868193)
Grant Information:: JP 16cm0106503 AMED P-CREATE; JP 16cm0106511 AMED P-CREATE; JP 17cm0106503 AMED P-CREATE; JP 17cm0106511 AMED P-CREATE; JP 18cm0106503 AMED P-CREATE; JP 18cm0106511 AMED P-CREATE; JP 19cm0106503 AMED P-CREATE; 19K07766 KAKENHI
Contributed Indexing:: Keywords: BRCAness; Lasso logistic regression; hereditary breast and ovarian cancer syndrome; homologous recombination deficiency; variants of uncertain significance
Substance Nomenclature:: 0 (BRCA1 Protein)
0 (BRCA1 protein, human)
0 (BRCA2 Protein)
0 (BRCA2 protein, human)
0 (Biomarkers, Tumor)
0 (Fanconi Anemia Complementation Group N Protein)
0 (PALB2 protein, human)
EC 2.7.1.11 (Checkpoint Kinase 2)
EC 2.7.11.1 (ATM protein, human)
EC 2.7.11.1 (Ataxia Telangiectasia Mutated Proteins)
EC 2.7.11.1 (CHEK2 protein, human)
Entry Date(s):: Date Created: 20210109 Date Completed: 20210317 Latest Revision: 20221207
Update Code:: 20240105
PubMed Central ID:: PMC7935793
DOI:: 10.1111/cas.14803
PMID:: 33421217
: Czasopismo naukowe

Full Text Finder

Genes involved in the homologous recombination repair pathway-as exemplified by BRCA1, BRCA2, PALB2, ATM, and CHEK2-are frequently associated with hereditary breast and ovarian cancer syndrome. Germline mutations in the loci of these genes with loss of heterozygosity or additional somatic truncation at the WT allele lead to the development of breast cancers with characteristic clinicopathological features and prominent genomic features of homologous recombination deficiency, otherwise referred to as "BRCAness." Although clinical genetic testing for these and other genes has increased the chances of identifying pathogenic variants, there has also been an increase in the prevalence of variants of uncertain significance, which poses a challenge to patient care because of the difficulties associated with making further clinical decisions. To overcome this challenge, we sought to develop a methodology to reclassify the pathogenicity of these unknown variants using statistical modeling of BRCAness. The model was developed with Lasso logistic regression by comparing 116 genomic attributes derived from 37 BRCA1/2 biallelic mutant and 32 homologous recombination-quiescent breast cancer exomes. The model showed 95.8% and 86.7% accuracies in the training cohort and The Cancer Genome Atlas validation cohort, respectively. Through application of the model for variant reclassification of homologous recombination-associated hereditary breast and ovarian cancer causal genes and further assessment with clinicopathological features, we finally identified one likely pathogenic and five likely benign variants. As such, the BRCAness model developed from the tumor exome was robust and provided a reasonable basis for variant reclassification.
(© 2021 The Authors. Cancer Science published by John Wiley & Sons Australia, Ltd on behalf of Japanese Cancer Association.)

Informacja