Prediction of BRCA1 and BRCA2 mutation status using post-irradiation assays of lymphoblastoid cell lines is compromised by inter-cell-line phenotypic variability

Assays to determine the pathogenicity of unclassified sequence variants in disease-associated genes include the analysis of lymphoblastoid cell lines (LCLs). We assessed the ability of several assays of LCLs to distinguish carriers of germline BRCA1 and BRCA2 gene mutations from mutation-negative co...

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Published in:	Breast cancer research and treatment Vol. 104; no. 3; pp. 257 - 266
Main Authors:	LOVELOCK, Paul K, EE MING WONG, BROWN, Melissa A, CHENEVIX-TRENCH, Georgia, SPURDLE, Amanda B, MCKAY, Michael J, SPRUNG, Carl N, MARSH, Anna, HOBSON, Karen, FRENCH, Juliet D, SOUTHEY, Melissa, INVESTIGATORS, Kconfab, SCULLEY, Tom, PANDEYA, Nirmala
Format:	Journal Article
Language:	English
Published:	Dordrecht Springer 01-09-2007 Springer Nature B.V
Subjects:	Biological and medical sciences Breast cancer Cancer research Cancer therapies Cell culture Cell Line, Tumor Cell Survival DNA Mutational Analysis Dose-Response Relationship, Radiation Genes Genes, BRCA1 Genes, BRCA2 Genetic Variation Genotype Genotype & phenotype Gynecology. Andrology. Obstetrics Humans Lymphocytes - radiation effects Mammary gland diseases Medical sciences Micronucleus Tests Mutation Phenotype Radiation therapy Radiation, Ionizing Telomere - metabolism Tumors Prediction Lymphoblastoid cell lines Post-IR metabolism BRCA1 Metabolism BRCA2 In vitro BRCA2 gene Established cell line Irradiation Phenotype variation Genetics Mutation Pharmacokinetics Predictive factor Lymphoblastoid cell BRCA1 gene Tumor suppressor gene
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Abstract	Assays to determine the pathogenicity of unclassified sequence variants in disease-associated genes include the analysis of lymphoblastoid cell lines (LCLs). We assessed the ability of several assays of LCLs to distinguish carriers of germline BRCA1 and BRCA2 gene mutations from mutation-negative controls to determine their utility for use in a diagnostic setting. Post-ionising radiation cell viability and micronucleus formation, and telomere length were assayed in LCLs carrying BRCA1 or BRCA2 mutations, and in unaffected mutation-negative controls. Post-irradiation cell viability and micronucleus induction assays of LCLs from individuals carrying pathogenic BRCA1 mutations, unclassified BRCA1 sequence variants or wildtype BRCA1 sequence showed significant phenotypic heterogeneity within each group. Responses were not consistent with predicted functional consequences of known pathogenic or normal sequences. Telomere length was also highly heterogeneous within groups of LCLs carrying pathogenic BRCA1 or BRCA2 mutations, and normal BRCA1 sequences, and was not predictive of mutation status. Given the significant degree of phenotypic heterogeneity of LCLs after gamma-irradiation, and the lack of association with BRCA1 or BRCA2 mutation status, we conclude that the assays evaluated in this study should not be used as a means of differentiating pathogenic and non-pathogenic sequence variants for clinical application. We suggest that a range of normal controls must be included in any functional assays of LCLs to ensure that any observed differences between samples reflect the genotype under investigation rather than generic inter-individual variation.
AbstractList	Assays to determine the pathogenicity of unclassified sequence variants in disease-associated genes include the analysis of lymphoblastoid cell lines (LCLs). We assessed the ability of several assays of LCLs to distinguish carriers of germline BRCA1 and BRCA2 gene mutations from mutation-negative controls to determine their utility for use in a diagnostic setting. Post-ionising radiation cell viability and micronucleus formation, and telomere length were assayed in LCLs carrying BRCA1 or BRCA2 mutations, and in unaffected mutation-negative controls. Post-irradiation cell viability and micronucleus induction assays of LCLs from individuals carrying pathogenic BRCA1 mutations, unclassified BRCA1 sequence variants or wildtype BRCA1 sequence showed significant phenotypic heterogeneity within each group. Responses were not consistent with predicted functional consequences of known pathogenic or normal sequences. Telomere length was also highly heterogeneous within groups of LCLs carrying pathogenic BRCA1 or BRCA2 mutations, and normal BRCA1 sequences, and was not predictive of mutation status. Given the significant degree of phenotypic heterogeneity of LCLs after gamma-irradiation, and the lack of association with BRCA1 or BRCA2 mutation status, we conclude that the assays evaluated in this study should not be used as a means of differentiating pathogenic and non-pathogenic sequence variants for clinical application. We suggest that a range of normal controls must be included in any functional assays of LCLs to ensure that any observed differences between samples reflect the genotype under investigation rather than generic inter-individual variation. BACKGROUND AND PURPOSE: Assays to determine the pathogenicity of unclassified sequence variants in disease-associated genes include the analysis of lymphoblastoid cell lines (LCLs). We assessed the ability of several assays of LCLs to distinguish carriers of germline BRCA1 and BRCA2 gene mutations from mutation-negative controls to determine their utility for use in a diagnostic setting. MATERIALS AND METHODS: Post-ionising radiation cell viability and micronucleus formation, and telomere length were assayed in LCLs carrying BRCA1 or BRCA2 mutations, and in unaffected mutation-negative controls. RESULTS: Post-irradiation cell viability and micronucleus induction assays of LCLs from individuals carrying pathogenic BRCA1 mutations, unclassified BRCA1 sequence variants or wildtype BRCA1 sequence showed significant phenotypic heterogeneity within each group. Responses were not consistent with predicted functional consequences of known pathogenic or normal sequences. Telomere length was also highly heterogeneous within groups of LCLs carrying pathogenic BRCA1 or BRCA2 mutations, and normal BRCA1 sequences, and was not predictive of mutation status. CONCLUSION: Given the significant degree of phenotypic heterogeneity of LCLs after gamma-irradiation, and the lack of association with BRCA1 or BRCA2 mutation status, we conclude that the assays evaluated in this study should not be used as a means of differentiating pathogenic and non-pathogenic sequence variants for clinical application. We suggest that a range of normal controls must be included in any functional assays of LCLs to ensure that any observed differences between samples reflect the genotype under investigation rather than generic inter-individual variation.
Author	INVESTIGATORS, Kconfab EE MING WONG FRENCH, Juliet D SCULLEY, Tom PANDEYA, Nirmala SPURDLE, Amanda B MCKAY, Michael J MARSH, Anna CHENEVIX-TRENCH, Georgia SPRUNG, Carl N LOVELOCK, Paul K SOUTHEY, Melissa HOBSON, Karen BROWN, Melissa A
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CitedBy_id	crossref_primary_10_1038_bjc_2014_391 crossref_primary_10_1016_j_ajhg_2012_04_019 crossref_primary_10_1002_mgg3_879 crossref_primary_10_1038_nrclinonc_2010_175 crossref_primary_10_1158_0008_5472_CAN_16_2568 crossref_primary_10_1038_sj_bjc_6605666 crossref_primary_10_1073_pnas_1110969108
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Keywords	Prediction Lymphoblastoid cell lines Post-IR metabolism BRCA1 Metabolism BRCA2 In vitro BRCA2 gene Established cell line Irradiation Phenotype variation Genetics Mutation Pharmacokinetics Predictive factor Lymphoblastoid cell BRCA1 gene Tumor suppressor gene
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Snippet	Assays to determine the pathogenicity of unclassified sequence variants in disease-associated genes include the analysis of lymphoblastoid cell lines (LCLs).... BACKGROUND AND PURPOSE: Assays to determine the pathogenicity of unclassified sequence variants in disease-associated genes include the analysis of... Background and purpose: Assays to determine the pathogenicity of unclassified sequence variants in disease-associated genes include the analysis of...
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SubjectTerms	Biological and medical sciences Breast cancer Cancer research Cancer therapies Cell culture Cell Line, Tumor Cell Survival DNA Mutational Analysis Dose-Response Relationship, Radiation Genes Genes, BRCA1 Genes, BRCA2 Genetic Variation Genotype Genotype & phenotype Gynecology. Andrology. Obstetrics Humans Lymphocytes - radiation effects Mammary gland diseases Medical sciences Micronucleus Tests Mutation Phenotype Radiation therapy Radiation, Ionizing Telomere - metabolism Tumors
Title	Prediction of BRCA1 and BRCA2 mutation status using post-irradiation assays of lymphoblastoid cell lines is compromised by inter-cell-line phenotypic variability
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