Your search keyword '"Eric C. Polley"' showing total 84 results

1. Contralateral Breast Cancer Risk Among Carriers of Germline Pathogenic Variants in ATM, BRCA1, BRCA2, CHEK2, and PALB2

Author

Siddhartha Yadav, Nicholas J. Boddicker, Jie Na, Eric C. Polley, Chunling Hu, Steven N. Hart, Rohan D. Gnanaolivu, Nicole Larson, Susan Holtegaard, Huaizhi Huang, Carolyn A. Dunn, Lauren R. Teras, Alpa V. Patel, James V. Lacey, Susan L. Neuhausen, Elena Martinez, Christopher Haiman, Fei Chen, Kathryn J. Ruddy, Janet E. Olson, Esther M. John, Allison W. Kurian, Dale P. Sandler, Katie M. O'Brien, Jack A. Taylor, Clarice R. Weinberg, Hoda Anton-Culver, Argyrios Ziogas, Gary Zirpoli, David E. Goldgar, Julie R. Palmer, Susan M. Domchek, Jeffrey N. Weitzel, Katherine L. Nathanson, Peter Kraft, and Fergus J. Couch

Subjects

Cancer Research, Oncology

Abstract

PURPOSE To estimate the risk of contralateral breast cancer (CBC) among women with germline pathogenic variants (PVs) in ATM, BRCA1, BRCA2, CHEK2, and PALB2. METHODS The study population included 15,104 prospectively followed women within the CARRIERS study treated with ipsilateral surgery for invasive breast cancer. The risk of CBC was estimated for PV carriers in each gene compared with women without PVs in a multivariate proportional hazard regression analysis accounting for the competing risk of death and adjusting for patient and tumor characteristics. The primary analyses focused on the overall cohort and on women from the general population. Secondary analyses examined associations by race/ethnicity, age at primary breast cancer diagnosis, menopausal status, and tumor estrogen receptor (ER) status. RESULTS Germline BRCA1, BRCA2, and CHEK2 PV carriers with breast cancer were at significantly elevated risk (hazard ratio > 1.9) of CBC, whereas only the PALB2 PV carriers with ER-negative breast cancer had elevated risks (hazard ratio, 2.9). By contrast, ATM PV carriers did not have significantly increased CBC risks. African American PV carriers had similarly elevated risks of CBC as non-Hispanic White PV carriers. Among premenopausal women, the 10-year cumulative incidence of CBC was estimated to be 33% for BRCA1, 27% for BRCA2, and 13% for CHEK2 PV carriers with breast cancer and 35% for PALB2 PV carriers with ER-negative breast cancer. The 10-year cumulative incidence of CBC among postmenopausal PV carriers was 12% for BRCA1, 9% for BRCA2, and 4% for CHEK2. CONCLUSION Women diagnosed with breast cancer and known to carry germline PVs in BRCA1, BRCA2, CHEK2, or PALB2 are at substantially increased risk of CBC and may benefit from enhanced surveillance and risk reduction strategies.

Published

2023

2. Germline Pathogenic Variants in Cancer Predisposition Genes Among Women With Invasive Lobular Carcinoma of the Breast

Author

Tina Pesaran, Jeffrey N. Weitzel, Clarice R. Weinberg, Chi Gao, Susan L. Neuhausen, Eric C. Polley, Alpa V. Patel, Christopher A. Haiman, Christine B. Ambrosone, Celine M. Vachon, Hongyan Huang, Sara Lindstrom, Julie R. Palmer, Esther M. John, Jill S. Dolinsky, Leslie Bernstein, Rohan Gnanaolivu, Allison W. Kurian, Steven N. Hart, Holly LaDuca, Hoda Anton-Culver, Janet E. Olson, Chunling Hu, Amal Yussuf, Song Yao, Nicole L. Larson, Peter Kraft, Jie Na, Fergus J. Couch, Nicholas J. Boddicker, Elena Martinez, Amy Trentham-Dietz, Siddhartha Yadav, Paul W. Auer, Dale R Sandler, Elizabeth C. Chao, Susan M. Domchek, Rachid Karam, Katherine L. Nathanson, James V. Lacey, Jack A. Taylor, and David E. Goldgar

Subjects

Adult, Cancer Research, Adolescent, Breast Neoplasms, Germline, Young Adult, Biomarkers, Tumor, Humans, Medicine, Genetic Predisposition to Disease, Genetic Testing, skin and connective tissue diseases, Gene, Germ-Line Mutation, Aged, Aged, 80 and over, business.industry, Cancer predisposition, Carcinoma, Ductal, Breast, ORIGINAL REPORTS, Middle Aged, Prognosis, medicine.disease, body regions, Carcinoma, Lobular, Oncology, Case-Control Studies, Invasive lobular carcinoma, cardiovascular system, Cancer research, Female, Hereditary Cancer, business, Follow-Up Studies

Abstract

PURPOSE To determine the contribution of germline pathogenic variants (PVs) in hereditary cancer testing panel genes to invasive lobular carcinoma (ILC) of the breast. MATERIALS AND METHODS The study included 2,999 women with ILC from a population-based cohort and 3,796 women with ILC undergoing clinical multigene panel testing (clinical cohort). Frequencies of germline PVs in breast cancer predisposition genes ( ATM, BARD1, BRCA1, BRCA2, BRIP1, CDH1, CHEK2, PALB2, PTEN, RAD51C, RAD51D, and TP53) were compared between women with ILC and unaffected female controls and between women with ILC and infiltrating ductal carcinoma (IDC). RESULTS The frequency of PVs in breast cancer predisposition genes among women with ILC was 6.5% in the clinical cohort and 5.2% in the population-based cohort. In case-control analysis, CDH1 and BRCA2 PVs were associated with high risks of ILC (odds ratio [OR] > 4) and CHEK2, ATM, and PALB2 PVs were associated with moderate (OR = 2-4) risks. BRCA1 PVs and CHEK2 p.Ile157Thr were not associated with clinically relevant risks (OR < 2) of ILC. Compared with IDC, CDH1 PVs were > 10-fold enriched, whereas PVs in BRCA1 were substantially reduced in ILC. CONCLUSION The study establishes that PVs in ATM, BRCA2, CDH1, CHEK2, and PALB2 are associated with an increased risk of ILC, whereas BRCA1 PVs are not. The similar overall PV frequencies for ILC and IDC suggest that cancer histology should not influence the decision to proceed with genetic testing. Similar to IDC, multigene panel testing may be appropriate for women with ILC, but CDH1 should be specifically discussed because of low prevalence and gastric cancer risk.

Published

2021

3. Risk of Late-Onset Breast Cancer in Genetically Predisposed Women

Author

Lauren R. Teras, Siddhartha Yadav, Amy Trentham-Dietz, Dale P. Sandler, James M. Hodge, Elena Ma Martínez, Fergus J. Couch, Jack A. Taylor, Katie M. O'Brien, Alpa V. Patel, Christopher A. Haiman, Chunling Hu, Mia M. Gaudet, David E. Goldgar, Paul W. Auer, James V. Lacey, Nicholas J. Boddicker, Sara Lindström, Celine M. Vachon, Susan L. Neuhausen, Irene M. Ong, Kimberly A. Bertrand, Leslie Bernstein, Loic Le Marchand, Eric C. Polley, Janet E. Olson, Hongyan Huang, Christine B. Ambrosone, Tina Pesaran, Susan M. Domchek, Amal Yussuf, Nicole L. Larson, Rohan Gnanaolivu, Brian D. Carter, Song Yao, Steven N. Hart, Holly LaDuca, Rachid Karam, Jie Na, Chi Gao, Katherine L. Nathanson, Peter Kraft, Elizabeth C. Chao, Huiyan Ma, Jeffrey N. Weitzel, Julie R. Palmer, Christopher E. Scott, Charles Kooperberg, Jill S. Dolinsky, David J. Hunter, and Elizabeth S. Burnside

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Population, MEDLINE, Breast Neoplasms, Late onset, Germline, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Internal medicine, RAPID COMMUNICATIONS, Biomarkers, Tumor, medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, Age of Onset, skin and connective tissue diseases, education, Germ-Line Mutation, Aged, Aged, 80 and over, BRCA2 Protein, education.field_of_study, BRCA1 Protein, business.industry, Prognosis, medicine.disease, Checkpoint Kinase 2, Germ Cells, 030104 developmental biology, Case-Control Studies, 030220 oncology & carcinogenesis, cardiovascular system, Female, Fanconi Anemia Complementation Group N Protein, business, Follow-Up Studies

Abstract

PURPOSE The prevalence of germline pathogenic variants (PVs) in established breast cancer predisposition genes in women in the general population over age 65 years is not well-defined. However, testing guidelines suggest that women diagnosed with breast cancer over age 65 years might have < 2.5% likelihood of a PV in a high-penetrance gene. This study aimed to establish the frequency of PVs and remaining risks of breast cancer for each gene in women over age 65 years. METHODS A total of 26,707 women over age 65 years from population-based studies (51.5% with breast cancer and 48.5% unaffected) were tested for PVs in germline predisposition gene. Frequencies of PVs and associations between PVs in each gene and breast cancer were assessed, and remaining lifetime breast cancer risks were estimated for non-Hispanic White women with PVs. RESULTS The frequency of PVs in predisposition genes was 3.18% for women with breast cancer and 1.48% for unaffected women over age 65 years. PVs in BRCA1, BRCA2, and PALB2 were found in 3.42% of women diagnosed with estrogen receptor (ER)–negative, 1.0% with ER-positive, and 3.01% with triple-negative breast cancer. Frequencies of PVs were lower among women with no first-degree relatives with breast cancer. PVs in CHEK2, PALB2, BRCA2, and BRCA1 were associated with increased risks (odds ratio = 2.9-4.0) of breast cancer. Remaining lifetime risks of breast cancer were ≥ 15% for those with PVs in BRCA1, BRCA2, and PALB2. CONCLUSION This study suggests that all women diagnosed with triple-negative breast cancer or ER-negative breast cancer should receive genetic testing and that women over age 65 years with BRCA1 and BRCA2 PVs and perhaps with PALB2 and CHEK2 PVs should be considered for magnetic resonance imaging screening.

Published

2021

4. Classification of BRCA2 variants of uncertain significance (VUS) using an ACMG/AMP model incorporating a homology directed repair (HDR) functional assay

Author

Chunling Hu, Lisa R. Susswein, Maegan E. Roberts, Hana Yang, Megan L. Marshall, Susan Hiraki, Windy Berkofsky-Fessler, Sounak Gupta, Wei Shen, Carolyn A. Dunn, Huaizhi Huang, Jie Na, Susan M. Domchek, Siddhartha Yadav, Alvaro N.A. Monteiro, Eric C. Polley, Steven N. Hart, Kathleen S. Hruska, and Fergus J. Couch

Subjects

BRCA2 Protein, Cancer Research, Oncology, Genes, BRCA2, Genetic Variation, Humans, Breast Neoplasms, Female, Genetic Predisposition to Disease, Genetic Testing, Article, Adenosine Monophosphate

Abstract

Purpose: The identification of variants of uncertain significance (VUS) in the BRCA1 and BRCA2 genes by hereditary cancer testing poses great challenges for the clinical management of variant carriers. The ACMG/AMP (American College of Medical Genetics and Genomics/Association for Molecular Pathology) variant classification framework, which incorporates multiple sources of evidence, has the potential to establish the clinical relevance of many VUS. We sought to classify the clinical relevance of 133 single-nucleotide substitution variants encoding missense variants in the DNA-binding domain (DBD) of BRCA2 by incorporating results from a validated functional assay into an ACMG/AMP-variant classification model from a hereditary cancer–testing laboratory. Experimental Design: The 133 selected VUS were evaluated using a validated homology-directed double-strand DNA break repair (HDR) functional assay. Results were combined with clinical and genetic data from variant carriers in a rules-based variant classification model for BRCA2. Results: Of 133 missense variants, 44 were designated as non-functional and 89 were designated as functional in the HDR assay. When combined with genetic and clinical information from a single diagnostic laboratory in an ACMG/AMP-variant classification framework, 66 variants previously classified by the diagnostic laboratory were correctly classified, and 62 of 67 VUS (92.5%) were reclassified as likely pathogenic (n = 22) or likely benign (n = 40). In total, 44 variants were classified as pathogenic/likely pathogenic, 84 as benign/likely benign, and 5 remained as VUS. Conclusions: Incorporation of HDR functional analysis into an ACMG/AMP framework model substantially improves BRCA2 VUS re-classification and provides an important tool for determining the clinical relevance of individual BRCA2 VUS.

Published

2022

5. Risk of Breast Cancer Among Carriers of Pathogenic Variants in Breast Cancer Predisposition Genes Varies by Polygenic Risk Score

Author

Amy Trentham-Dietz, Katie M. O'Brien, Alpa V. Patel, Rohan Gnanaolivu, Chi Gao, Katherine L. Nathanson, Lauren R. Teras, Clarice R. Weinberg, Nicholas J. Boddicker, David J. Hunter, Julie R. Palmer, Polly A. Newcomb, Jeffrey N. Weitzel, Eric J. Jacobs, Dale P. Sandler, Jenna Lilyquist, Leslie Bernstein, Rulla M. Tamimi, Christine B. Ambrosone, Fergus J. Couch, Celine M. Vachon, Esther M. John, Christopher A. Haiman, Jack A. Taylor, Hongyan Huang, Mia M. Gaudet, David E. Goldgar, Irene M. Ong, Susan M. Domchek, Chunling Hu, Sara Lindström, Jie Na, Elizabeth S. Burnside, Susan L. Neuhausen, Janet E. Olson, Eric C. Polley, Song Yao, Peter Kraft, Huiyan Ma, Steven N. Hart, A. Heather Eliassen, and Paul L. Auer

Subjects

Adult, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, MEDLINE, Breast Neoplasms, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Risk Factors, Internal medicine, medicine, Humans, Genetic Predisposition to Disease, Gene, Aged, business.industry, Genetic Variation, ORIGINAL REPORTS, Middle Aged, medicine.disease, 030104 developmental biology, 030220 oncology & carcinogenesis, Female, Polygenic risk score, business

Abstract

PURPOSE This study assessed the joint association of pathogenic variants (PVs) in breast cancer (BC) predisposition genes and polygenic risk scores (PRS) with BC in the general population. METHODS A total of 26,798 non-Hispanic white BC cases and 26,127 controls from predominately population-based studies in the Cancer Risk Estimates Related to Susceptibility consortium were evaluated for PVs in BRCA1, BRCA2, ATM, CHEK2, PALB2, BARD1, BRIP1, CDH1, and NF1. PRS based on 105 common variants were created using effect estimates from BC genome-wide association studies; the performance of an overall BC PRS and estrogen receptor–specific PRS were evaluated. The odds of BC based on the PVs and PRS were estimated using penalized logistic regression. The results were combined with age-specific incidence rates to estimate 5-year and lifetime absolute risks of BC across percentiles of PRS by PV status and first-degree family history of BC. RESULTS The estimated lifetime risks of BC among general-population noncarriers, based on 10th and 90th percentiles of PRS, were 9.1%-23.9% and 6.7%-18.2% for women with or without first-degree relatives with BC, respectively. Taking PRS into account, more than 95% of BRCA1, BRCA2, and PALB2 carriers had > 20% lifetime risks of BC, whereas, respectively, 52.5% and 69.7% of ATM and CHEK2 carriers without first-degree relatives with BC, and 78.8% and 89.9% of those with a first-degree relative with BC had > 20% risk. CONCLUSION PRS facilitates personalization of BC risk among carriers of PVs in predisposition genes. Incorporating PRS into BC risk estimation may help identify > 30% of CHEK2 and nearly half of ATM carriers below the 20% lifetime risk threshold, suggesting the addition of PRS may prevent overscreening and enable more personalized risk management approaches.

Published

2021

6. Abstract GS4-04: Population-based Estimates of contralateral Breast Cancer Risk among Carriers of Germline Pathogenic Variants in ATM, BRCA1, BRCA2, CHEK2, and PALB2

Author

Siddhartha Yadav, Nicholas J. Boddicker, Jie Na, Eric C. Polley, Chunling Hu, Steven N. Hart, Rohan D. Gnanaolivu, Nicole Larson, Carolyn Dunn, Susan Holtegaard, Huaizhi Huang, Lauren R. Teras, Alpa V. Patel, James V. Lacey, Susan Neuhausen, Leslie Bernstein, Elena Martinez, Christopher Haiman, Fei Chen, Kathryn Ruddy, Janet Olson, Esther John, Allison W. Kurian, Dale P. Sandler, Katie M. O’Brien, Jack A. Taylor, Clarice R. Weinberg, Hoda Anton-Culver, Argyrios Ziogas, Gary R. Zirpoli, David E. Goldgar, Katherine L. Nathanson, Susan Domchek, Julie R. Palmer, Jeffrey Weitzel, Peter Kraft, and Fergus J. Couch

Subjects

Cancer Research, Oncology

Abstract

Purpose To estimate the risk of contralateral breast cancer (CBC) among women in the general population with germline pathogenic variants (PVs) in ATM, BRCA1, BRCA2, CHEK2, and PALB2. Methods Among 15,104 prospectively followed women within the CARRIERS study treated with ipsilateral surgery for invasive breast cancer, a subset of 14,237 women were identified from population-based studies. The risk of CBC was estimated for PV carriers in each gene compared to women without PVs in a multivariate proportional hazard regression analysis accounting for the competing risk of death and adjusting for patient and tumor characteristics. The primary analyses focused on the overall cohort and on women from the general population. Secondary analyses examined associations by race/ethnicity, age at primary breast cancer diagnosis, menopausal status, and tumor estrogen receptor status. Results Germline BRCA1, BRCA2, and CHEK2 PV carriers with breast cancer were at significantly elevated risk (Hazard ratio ≥ 1.9, p< 0.05) of CBC, whereas only the PALB2 PV carriers with ER-negative breast cancer had elevated risks. In contrast, ATM PV carriers did not have significantly increased CBC risks. African American PV carriers had similarly elevated risks of CBC as non-Hispanic White PV carriers. Among premenopausal women, the 15-year cumulative incidence of CBC was >20% for BRCA1, BRCA2 and CHEK2 PV carriers with breast cancer, and for PALB2 PV carriers with ER-negative breast cancer. The 15-year cumulative incidence of CBC among postmenopausal PV carriers was < 20% for PV carriers in any of the 5 genes. Conclusions Women diagnosed with breast cancer and known to carry germline PVs in BRCA1, BRCA2, CHEK2, or PALB2 are at substantially increased risk of CBC and may benefit from enhanced surveillance and risk-reduction strategies. Citation Format: Siddhartha Yadav, Nicholas J. Boddicker, Jie Na, Eric C. Polley, Chunling Hu, Steven N. Hart, Rohan D. Gnanaolivu, Nicole Larson, Carolyn Dunn, Susan Holtegaard, Huaizhi Huang, Lauren R. Teras, Alpa V. Patel, James V. Lacey Jr., Susan Neuhausen, Leslie Bernstein, Elena Martinez, Christopher Haiman, Fei Chen, Kathryn Ruddy, Janet Olson, Esther John, Allison W. Kurian, Dale P. Sandler, Katie M. O’Brien, Jack A. Taylor, Clarice R. Weinberg, Hoda Anton-Culver, Argyrios Ziogas, Gary R. Zirpoli, David E. Goldgar, Katherine L. Nathanson, Susan Domchek, Julie R. Palmer, Jeffrey Weitzel, Peter Kraft, Fergus J. Couch. Population-based Estimates of contralateral Breast Cancer Risk among Carriers of Germline Pathogenic Variants in ATM, BRCA1, BRCA2, CHEK2, and PALB2 [abstract]. In: Proceedings of the 2022 San Antonio Breast Cancer Symposium; 2022 Dec 6-10; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2023;83(5 Suppl):Abstract nr GS4-04.

Published

2023

7. Effect of Germline Mutations in Homologous Recombination Repair Genes on Overall Survival of Patients with Pancreatic Adenocarcinoma

Author

Thanh P. Ho, Eric C. Polley, Robert R. McWilliams, William R. Bamlet, Steven N. Hart, Kari G. Rabe, Nicholas J. Boddicker, Pashtoon Murtaza Kasi, Fergus J. Couch, Chunling Hu, Siddhartha Yadav, Kun Y. Lee, Gloria M. Petersen, Tricia Lindstrom, and Rohan Gnanaolivu

Subjects

Male, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, PALB2, Adenocarcinoma, medicine.disease_cause, Article, Germline, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, BARD1, Internal medicine, Biomarkers, Tumor, Humans, Medicine, Genetic Testing, Prospective Studies, Germ-Line Mutation, Aged, Mutation, business.industry, BRIP1, Recombinational DNA Repair, Middle Aged, Prognosis, medicine.disease, Pancreatic Neoplasms, Survival Rate, DNA Repair Enzymes, 030104 developmental biology, 030220 oncology & carcinogenesis, RAD51C, Female, business, Follow-Up Studies

Abstract

Purpose:To compare the clinical characteristics and overall survival (OS) of germline mutation carriers in homologous recombination repair (HRR) genes and noncarriers with pancreatic ductal adenocarcinoma (PDAC).Experimental Design:Germline DNA from 3,078 patients with PDAC enrolled in a prospective registry at Mayo Clinic between 2000 and 2017 was analyzed for mutations in 37 cancer predisposition genes. Characteristics and OS of patients with mutations in eight genes (ATM, BARD1, BRCA1, BRCA2, BRIP1, PALB2, RAD51C, and RAD51D) involved in HRR were compared with patients testing negative for mutations in all 37 genes.Results:The 175 HRR mutation carriers and 2,730 noncarriers in the study had a median duration of follow-up of 9.9 years. HRR mutation carriers were younger (median age at diagnosis: 63 vs. 66 years, P < 0.001) and more likely to have metastatic disease at diagnosis (46% vs. 36%, P = 0.004). In a multivariable model adjusting for sex, age at diagnosis, and tumor staging, patients with germline HRR mutations had a significantly longer OS compared with noncarriers [HR, 0.83; 95% confidence interval (CI), 0.70–0.97; P = 0.02]. Further gene-level analysis demonstrated that germline ATM mutation carriers had longer OS compared with patients without germline mutations in any of the 37 genes (HR, 0.72; 95% CI, 0.55–0.94; P = 0.01).Conclusions:This study demonstrates that germline mutation carrier status in PDAC is associated with longer OS compared with noncarriers. Further research into tumor biology and response to platinum-based chemotherapy in germline mutation carriers with PDAC are needed to better understand the association with longer OS.

Published

2020

8. Racial and Ethnic Differences in Multigene Hereditary Cancer Panel Test Results for Women With Breast Cancer

Author

Jill S. Dolinsky, Brigette Tippin Davis, David E. Goldgar, Tina Pesaran, Jenna Lilyquist, Jie Na, Holly LaDuca, Amal Yussuf, Nancy Niguidula, Elizabeth C. Chao, Chunling Hu, Hermela Shimelis, Steven N. Hart, Siddhartha Yadav, Fergus J. Couch, Kun Y. Lee, Stephanie Gutierrez, and Eric C. Polley

Subjects

Cancer Research, 2019-20 coronavirus outbreak, Ethnic group, Breast Neoplasms, Brief Communication, 03 medical and health sciences, Race (biology), 0302 clinical medicine, Breast cancer, Ethnicity, Humans, Medicine, Genetic Predisposition to Disease, CHEK2, 030304 developmental biology, 0303 health sciences, business.industry, Hispanic or Latino, medicine.disease, Ashkenazi jews, Increased risk, Oncology, Case-Control Studies, 030220 oncology & carcinogenesis, cardiovascular system, Female, Hereditary Cancer, AcademicSubjects/MED00010, business, Demography

Abstract

To evaluate the racial and ethnic differences in prevalence of germline pathogenic variants (PVs) and the effect of race and ethnicity on breast cancer (BC) risk among carriers, results of multigene testing of 77 900 women with BC (non-Hispanic White [NHW] = 57 003; Ashkenazi-Jewish = 4798; Black = 6722; Hispanic = 5194; and Asian = 4183) were analyzed, and the frequency of PVs in each gene were compared between BC patients (cases) and race- and ethnicity-matched gnomAD reference controls. Compared with NHWs, BRCA1 PVs were enriched in Ashkenazi-Jews and Hispanics, whereas CHEK2 PVs were statistically significantly lower in Blacks, Hispanics, and Asians (all 2-sided P 4.00) of BC in Blacks, Hispanics, and Asians; ATM PVs were associated with increased risk of BC among all races and ethnicities except Asians, whereas CHEK2 and BRIP1 PVs were associated with increased risk of BC among NHWs and Hispanics only. These findings suggest a need for personalized management of BC risk in PV carriers based on race and ethnicity.

Published

2020

9. Contribution of Germline Predisposition Gene Mutations to Breast Cancer Risk in African American Women

Author

Loic LeMarchand, Esther M. John, Song Yao, Mia M. Gaudet, Chi Gao, Tuya Pal, Julie R. Palmer, Kimberly A. Bertrand, Payal D. Shah, Rohan Gnanaolivu, Katherine L. Nathanson, Chunling Hu, Susan M. Domchek, Peter Kraft, Jie Na, Leslie Bernstein, Fergus J. Couch, David E Goldgar, Eric C. Polley, Elisa V. Bandera, Dale P. Sandler, Christine B. Ambrosone, Jeffrey N. Weitzel, Amy Trentham-Dietz, Siddhartha Yadav, Steven N. Hart, William Yang, Kun Y. Lee, Christopher A. Haiman, Traci N. Bethea, Hongyan Huang, and Hoda Anton-Culver

Subjects

Oncology, 0303 health sciences, Cancer Research, medicine.medical_specialty, education.field_of_study, medicine.diagnostic_test, business.industry, PALB2, Population, Estrogen receptor, Cancer, Gene mutation, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, 030220 oncology & carcinogenesis, Internal medicine, medicine, business, education, CHEK2, 030304 developmental biology, Genetic testing

Abstract

Background The risks of breast cancer in African American (AA) women associated with inherited mutations in breast cancer predisposition genes are not well defined. Thus, whether multigene germline hereditary cancer testing panels are applicable to this population is unknown. We assessed associations between mutations in panel-based genes and breast cancer risk in 5054 AA women with breast cancer and 4993 unaffected AA women drawn from 10 epidemiologic studies. Methods Germline DNA samples were sequenced for mutations in 23 cancer predisposition genes using a QIAseq multiplex amplicon panel. Prevalence of mutations and odds ratios (ORs) for associations with breast cancer risk were estimated with adjustment for study design, age, and family history of breast cancer. Results Pathogenic mutations were identified in 10.3% of women with estrogen receptor (ER)-negative breast cancer, 5.2% of women with ER-positive breast cancer, and 2.3% of unaffected women. Mutations in BRCA1, BRCA2, and PALB2 were associated with high risks of breast cancer (OR = 47.55, 95% confidence interval [CI] = 10.43 to >100; OR = 7.25, 95% CI = 4.07 to 14.12; OR = 8.54, 95% CI = 3.67 to 24.95, respectively). RAD51D mutations were associated with high risk of ER-negative disease (OR = 7.82, 95% CI = 1.61 to 57.42). Moderate risks were observed for CHEK2, ATM, ERCC3, and FANCC mutations with ER-positive cancer, and RECQL mutations with all breast cancer. Conclusions The study identifies genes that predispose to breast cancer in the AA population, demonstrates the validity of current breast cancer testing panels for use in AA women, and provides a basis for increased referral of AA patients for cancer genetic testing.

Published

2020

10. Evaluation of Germline Genetic Testing Criteria in a Hospital-Based Series of Women With Breast Cancer

Author

Prema P. Peethambaram, Patrick D. Fitz-Gibbon, Siddhartha Yadav, Daniela L. Stan, Sandhya Pruthi, Nicole P. Sandhu, Nicholas J. Boddicker, Sebastian M. Armasu, Judy C. Boughey, Karthik Ghosh, Janet E. Olson, Eric C. Polley, Christine L. Klassen, Kathryn J. Ruddy, Tufia C. Haddad, Deborah J. Rhodes, Rohan Gnanaolivu, Lonzetta Neal, Kun Y. Lee, Steven N. Hart, Matthew P. Goetz, Susan M. Domchek, Chunling Hu, Tanya L. Hoskin, Jie Na, Fergus J. Couch, and Tricia Lindstrom

Subjects

0301 basic medicine, Oncology, Adult, Cancer Research, medicine.medical_specialty, Genetic Testing for Cancer, MEDLINE, Breast Neoplasms, Sensitivity and Specificity, Germline, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Breast cancer, Internal medicine, Medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, skin and connective tissue diseases, Germ-Line Mutation, Genetic testing, Aged, Aged, 80 and over, BRCA2 Protein, medicine.diagnostic_test, business.industry, BRCA1 Protein, Reproducibility of Results, Hospital based, ORIGINAL REPORTS, Middle Aged, medicine.disease, Hospitals, 030104 developmental biology, 030220 oncology & carcinogenesis, Female, business, Fanconi Anemia Complementation Group N Protein

Abstract

PURPOSE To determine the sensitivity and specificity of genetic testing criteria for the detection of germline pathogenic variants in women with breast cancer. MATERIALS AND METHODS Women with breast cancer enrolled in a breast cancer registry at a tertiary cancer center between 2000 and 2016 were evaluated for germline pathogenic variants in 9 breast cancer predisposition genes ( ATM , BRCA1, BRCA2, CDH1, CHEK2, NF1, PALB2, PTEN, and TP53). The performance of the National Comprehensive Cancer Network (NCCN) hereditary cancer testing criteria was evaluated relative to testing of all women as recommended by the American Society of Breast Surgeons. RESULTS Of 3,907 women, 1,872 (47.9%) meeting NCCN criteria were more likely to carry a pathogenic variant in 9 predisposition genes compared with women not meeting criteria (9.0% v 3.5%; P < .001). Of those not meeting criteria (n = 2,035), 14 (0.7%) had pathogenic variants in BRCA1 or BRCA2. The sensitivity of NCCN criteria was 70% for 9 predisposition genes and 87% for BRCA1 and BRCA2, with a specificity of 53%. Expansion of the NCCN criteria to include all women diagnosed with breast cancer at ≤ 65 years of age achieved > 90% sensitivity for the 9 predisposition genes and > 98% sensitivity for BRCA1 and BRCA2. CONCLUSION A substantial proportion of women with breast cancer carrying germline pathogenic variants in predisposition genes do not qualify for testing by NCCN criteria. Expansion of NCCN criteria to include all women diagnosed at ≤ 65 years of age improves the sensitivity of the selection criteria without requiring testing of all women with breast cancer.

Published

2020

11. Abstract A003: Risks of ductal carcinoma in situ of the breast associated with pathogenic variants in cancer predisposition genes

Author

Huaizhi Huang, Ronan E. Couch, Holly LaDuca, Siddhartha Yadav, Eric C. Polley, Nicholas J. Boddicker, Jie Na, Rohan D. Gnanaolivu, David E. Goldgar, Tina Pesaran, Steven N. Hart, Jill S. Dolinsky, Julie R. Palmer, Lauren Teras, Alpa V. Patel, Kathryn J. Ruddy, Janet E. Olson, Celine M. Vachon, Peter Kraft, Song Yao, Amy Trentham-Dietz, Katherine L. Nathanson, Jeffrey N. Weitzel, Susan M. Domchek, Fergus J. Couch, and Chunling Hu

Subjects

Cancer Research, Oncology

Abstract

Introduction: The relationship between germline pathogenic variants (PVs) in cancer predisposition genes and ductal carcinoma in situ (DCIS) is not well established. The objective of this study is to determine the risks of DCIS and contralateral breast cancer among women with DCIS associated with germline PVs in cancer predisposition genes. Methods: Associations between pathogenic variants in 11 cancer predisposition genes (ATM, BARD1, BRCA1, BRCA2, BRIP1, CDH1, CHEK2, MSH6, PALB2, RAD51C, and RAD51D) and DCIS were determined in case control analyses of a population-based cohort of 3876 women with DCIS and age-matched unaffected women, and in a clinical cohort of 9887 DCIS cases undergoing clinical genetic testing at Ambry Genetics and unaffected reference controls. The incidence of contralateral breast cancer risk in BRCA1, BRCA2, and PALB2 PV carriers with DCIS was also evaluated in a time-to-event analysis. Results: The mean age at diagnosis of DCIS was 50 years in the clinical testing cohort and 59 years in the population-based cohort. The frequency of PVs in 11 predisposition genes among DCIS cases was 6.9% in the clinical testing cohort and 4.9% in the population-based cohort. PVs in ATM, BRCA1, BRCA2, CHEK2, MSH6, PALB2, and RAD51D were associated with significantly increased risks (Odds Ratio (OR) >2) of DCIS in the clinical testing cohort whereas only PVs in BRCA1, CHEK2, PALB2, and ATM were associated with significantly increased risks of DCIS in the population-based cohort. The cumulative incidence of contralateral breast cancer among BRCA1, BRCA2, and PALB2 PV carriers with DCIS was 11% in 5-years and 20% in 15-years. Conclusions: This study provides new insights into PVs that predispose to DCIS. In addition, it establishes an increased risk of contralateral breast cancer risk among women with DCIS who are carriers of PVs in BRCA1, BRCA2, or PALB2. These findings will guide surveillance and risk reducing strategies in germline PV carriers with DCIS. Citation Format: Huaizhi Huang, Ronan E. Couch, Holly LaDuca, Siddhartha Yadav, Eric C. Polley, Nicholas J. Boddicker, Jie Na, Rohan D. Gnanaolivu, David E. Goldgar, Tina Pesaran, Steven N. Hart, Jill S. Dolinsky, Julie R. Palmer, Lauren Teras, Alpa V. Patel, Kathryn J. Ruddy, Janet E. Olson, Celine M. Vachon, Peter Kraft, Song Yao, Amy Trentham-Dietz, Katherine L. Nathanson, Jeffrey N. Weitzel, Susan M. Domchek, Fergus J. Couch, Chunling Hu. Risks of ductal carcinoma in situ of the breast associated with pathogenic variants in cancer predisposition genes [abstract]. In: Proceedings of the AACR Special Conference on Rethinking DCIS: An Opportunity for Prevention?; 2022 Sep 8-11; Philadelphia, PA. Philadelphia (PA): AACR; Can Prev Res 2022;15(12 Suppl_1): Abstract nr A003.

Published

2022

12. Abstract P5-07-06: Performance of a polygenic risk score combined with clinical assessment for breast cancer risk

Author

Shuwei Li, Sebastian M. Armasu, Christopher G. Scott, Patrick D. Fitz-Gibbon, Mary Helen Black, Celine M. Vachon, Janet E. Olson, Fergus J. Couch, Eric C. Polley, Holly LaDuca, Kathryn J. Ruddy, and Stacey J. Winham

Subjects

Oncology, Cancer Research, medicine.medical_specialty, education.field_of_study, business.industry, Medical record, Population, Cancer, Odds ratio, medicine.disease, Logistic regression, Breast cancer, Internal medicine, medicine, Family history, Ovarian cancer, business, education

Abstract

Background: Polygenic risk scores (PRS) based on a large number of SNPs associated with breast cancer have recently been made available in combination with multigene panel testing for clinical management of breast cancer risk. Breast cancer risk assessment has historically been performed using various non-genetic risk models, which predict lifetime risk of breast cancer in unaffected women based on personal and family history information. While clinical use of PRS in combination with these models continues to increase, the predictive performance of a PRS combined with clinical information in real-world patient populations has not been thoroughly investigated. Methods: We assessed a 100-SNP breast cancer PRS in combination with the Tyrer-Cuzick model-estimated lifetime breast cancer risk in 5,374 Caucasian women from the case-control Mayo Clinic Breast Cancer Study (MCBCS), comprised of 3,373 breast cancer cases and 2,001 unaffected controls seen at Mayo Clinic from 2004 to 2016. Clinical, family history, and demographic information was collected on all MCBCS participants via questionnaires and medical record review. SNPs were selected for the PRS if they exceeded genome-wide significance in ≥2 large-scale breast cancer genome wide association studies (GWAS) in women of European descent. Selected SNPs were then used to construct a population standardized PRS, accounting for per-allele odds ratios reported in the largest GWAS to date and population-specific allele frequencies. PRS and Tyrer-Cuzick model associations with breast cancer and related clinical features were tested using multivariate logistic regression. Results: Among cases and controls, mean±SD age at diagnosis and study enrollment was 56.4±12.4 and 56.2±14.1, respectively. Approximately 36.9% of cases and 16.9% of controls had ≥1 first- or second-degree relative with breast or ovarian cancer, respectively. Among unaffected women, the median (IQR) estimated lifetime risk of breast cancer to age 85 based on Tyrer-Cuzick alone was 8.3% (6.9%), and 2.6% had a clinically actionable lifetime risk of ≥20%. The mean±SD sum of the risk alleles across 100 SNPs was significantly higher for cases vs. controls (94.8±6.3 vs. 92.7±6.2, p Citation Format: Mary Helen Black, Shuwei Li, Holly LaDuca, Sebastian Armasu, Eric C. Polley, Patrick Fitz-Gibbon, Chris G. Scott, Stacey J. Winham, Janet E. Olson, Kathryn J. Ruddy, Celine M. Vachon, Fergus J. Couch. Performance of a polygenic risk score combined with clinical assessment for breast cancer risk [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr P5-07-06.

Published

2020

13. Abstract P6-08-01: Comparison of recommendations for germline genetic testing in an unselected cohort of patients with breast cancer

Author

Steven N. Hart, Chunling Hu, Fergus J. Couch, Jie Na, Siddhartha Yadav, Nicholas J. Boddicker, Eric C. Polley, Kun Y. Lee, Janet E. Olson, Kathryn J. Ruddy, and Rohan Gnanaolivu

Subjects

Oncology, Cancer Research, medicine.medical_specialty, medicine.diagnostic_test, business.industry, medicine.disease, Germline, Breast cancer, Internal medicine, Cohort, Medicine, business, Genetic testing

Abstract

Purpose: To determine the sensitivity of germline hereditary cancer genetic testing recommendations for detection of pathogenic mutations in breast cancer predisposition genes in an unselected cohort of breast cancer patients. Patients and Methods: The study population included patients enrolled in a prospective breast cancer registry after being seen at Mayo Clinic for newly diagnosed breast cancer between 2004 and 2016. All patients were subjected to germline mutation testing for 12 known breast cancer predisposition genes (ATM, BARD1, BRCA1, BRCA2, CDH1, CHEK2, NF1, PALB2, PTEN, RAD51C, RAD51D and TP53). Results from testing of all breast cancer patients according to American Society of Breast Surgeons (ASBrS) genetic testing recommendations and patients meeting National Comprehensive Cancer Network (NCCN) criteria for BRCA1/2 testing, based on age at diagnosis and personal and family history of cancer, were compared. Results: Among the 4516 patients in the cohort, the median age at diagnosis of breast cancer was 57 years, 80.5% had estrogen receptor positive tumors, and 43% had a family history of breast cancer. All patients in the cohort met ASBrS criteria for hereditary cancergenetic testing, 2050 (45.4%) met NCCN criteria, 1892 (41.9%) did not meet NCCN criteria, and 574 (12.7%) patients could not be fully evaluated for NCCN testing criteria due to missing data. The frequencies of pathogenic variants in the cohort are shown in Table 1. Patients meeting NCCN criteria were more likely to carry a pathogenic variant compared to those who did not (9.8% vs. 3.8%, p When testing was expanded to include all patients with breast cancer diagnosed at age ≤65 and/or meeting NCCN testing criteria, only 20 (7.4%) out of 272 mutation carriers in 12 breast cancer genes and 2 (1.6%) out of 121 BRCA1/2 mutation carriers were overlooked. However, this increased the number tested to detect one mutation carrier on average from 17 to 25 for BRCA1/2 and from 9 to 12 for the 12 breast cancer predisposition genes. In total, this age cutoff led to an increase in the number of patients tested by 28% while the number of patients in the cohort that need not undergo germline genetic testing was 20%. Conclusions: Although NCCN criteria for BRCA1/2 germline genetic testing detect the majority of predisposition gene mutation carriers, a significant number of carriers are missed in an unselected cohort of breast cancer patients using these criteria. Expanding the current NCCN criteria to include all women with breast cancer diagnosed ≤ 65 years of age, will substantially improve the sensitivity of mutation testing, without the need for evaluation of all breast cancer patients. Table 1: Comparison of frequency of germline mutations between patients who met and did not meet NCCN guidelines for germline genetic testing#Total, Meets ASBrS guidelines N=3942Meets NCCN guidelines, N=2050Did not meet NCCN guidelines, N=1892P-value€ NCCN vs non-NCCNPercent mutation carriers missed by NCCN criteria* BRCA1/2121 (3.1%)106 (5.2%)15 (0.8%) Citation Format: Siddhartha Yadav, Chunling Hu, Steven N. Hart, Nicholas Boddicker, Eric C. Polley, Jie Na, Rohan Gnanaolivu, Kun Y. Lee, Janet E. Olson, Kathryn J. Ruddy, Fergus J. Couch. Comparison of recommendations for germline genetic testing in an unselected cohort of patients with breast cancer [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr P6-08-01.

Published

2020

14. Abstract P6-08-04: Germline mutations in cancer predisposition genes in patients with invasive lobular carcinoma of the breast

Author

Brandon Smith, Tina Pesaran, Fergus J. Couch, Eric C. Polley, Jill S. Dolinsky, Jie Na, Chunling Hu, David E. Goldgar, Siddhartha Yadav, Rohan Gnanaolivu, Holly LaDuca, and Steven N. Hart

Subjects

Cancer Research, Germline mutation, Oncology, business.industry, Cancer predisposition, Invasive lobular carcinoma, Cancer research, Medicine, In patient, business, medicine.disease, Gene

Abstract

Background: Invasive lobular carcinoma (ILC) of the breast accounts for approximately 10-15% of all histologic subtypes of breast cancer. However, apart from germline mutations in CDH1, the contributions of mutations in other cancer predisposition genes to ILC are largely unknown. Methods: The study population included 3,893 women with ILC of the breast who underwent germline multigene panel testing of cancer predisposition genes at Ambry Genetics from March 2012 to December 2016. The prevalence of predisposition gene mutations in women with ILC was assessed relative to 38,004 women with invasive ductal carcinoma (IDC) who underwent germline multigene panel testing at Ambry Genetics during the same timeframe. Associations between mutations in each gene and risk of ILC were evaluated using reference controls. Results: Of the 3,893 women with ILC included in this study, 70.7% were non-Hispanic white, 65.1% had a family history of breast cancer, and 96.4% had estrogen receptor (ER) positive breast cancer. The overall frequency of germline mutations in cancer predisposition genes (ATM, BARD1, BRCA1, BRCA2, BRIP1, CDH1, CDKN2A, CHEK2, MLH1, MRE11A, MSH2, MSH6, NBN, NF1, PALB2, PTEN, RAD51C, RAD51D and TP53) was 7.8% for women with ILC and 10.7% for women with IDC. Mutations in CDH1 were significantly more frequent (Odds Ratio (OR)=12.1, p2), NBN mutations were associated with ILC (OR=3.4; p Conclusions: In a large cohort of patients with ILC, the frequencies of germline mutations in cancer predisposition genes were similar between ILC and IDC except for ATM, BRCA1, CDH1 and PALB2. Six genes, in addition to CDH1, were found to be germline predisposition genes for ILC. A substantial proportion of patients older than 50 with ILC without a family history of breast or ovarian cancer or a personal history of other cancers were found to be mutation carriers. These findings improve our understanding of germline genetic drivers of ILC and suggest that multigene genetic testing should be considered for all ILC patients. Citation Format: Siddhartha Yadav, Holly LaDuca, Eric C. Polley, Chunling Hu, Steven N. Hart, Jie Na, Rohan Gnanaolivu, Brandon Smith, David E Goldgar, Tina Pesaran, Jill S. Dolinsky, Fergus J. Couch. Germline mutations in cancer predisposition genes in patients with invasive lobular carcinoma of the breast [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr P6-08-04.

Published

2020

15. Gene expression differences between matched pairs of ovarian cancer patient tumors and patient-derived xenografts

Author

Paul Haluska, Cordelia D. McGehee, Ellen L. Goode, Jaime I. Davila, Valentina Zanfagnin, S. John Weroha, Yuanhang Liu, Xiaonan Hou, Pritha Chanana, Chen Wang, and Eric C. Polley

Subjects

0301 basic medicine, endocrine system, Stromal cell, endocrine system diseases, lcsh:Medicine, PDGFRB, PDGFRA, Biology, digestive system, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Stroma, Ovarian cancer, Gene expression, Cancer genomics, medicine, Animals, Humans, lcsh:Science, Gene, Ovarian Neoplasms, Regulation of gene expression, Multidisciplinary, lcsh:R, nutritional and metabolic diseases, medicine.disease, Computational biology and bioinformatics, Neoplasm Proteins, 3. Good health, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Cancer research, Heterografts, Female, lcsh:Q, Neoplasm Transplantation, 030217 neurology & neurosurgery, hormones, hormone substitutes, and hormone antagonists

Abstract

As patient derived xenograft (PDX) models are increasingly used for preclinical drug development, strategies to account for the nonhuman component of PDX RNA expression data are critical to its interpretation. A bioinformatics pipeline to separate donor tumor and mouse stroma transcriptome profiles was devised and tested. To examine the molecular fidelity of PDX versus donor tumors, we compared mRNA differences between paired PDX-donor tumors from nine ovarian cancer patients. 1,935 differentially expressed genes were identified between PDX and donor tumors. Over 90% (n = 1767) of these genes were down-regulated in PDX models and enriched in stroma-specific functions. Several protein kinases were also differentially expressed in PDX tumors, e.g. PDGFRA, PDGFRB and CSF1R. Upon in silico removal of these PDX-donor tumor differentially expressed genes, a stronger transcriptional resemblance between PDX-donor tumor pairs was seen (average correlation coefficient increases from 0.91 to 0.95). We devised and validated an effective bioinformatics strategy to separate mouse stroma expression from human tumor expression for PDX RNAseq. In addition, we showed most of the PDX-donor differentially expressed genes were implicated in stromal components. The molecular similarities and differences between PDX and donor tumors have implications in future therapeutic trial designs and treatment response evaluations using PDX models.

Published

2019

16. Systemic treatment and radiotherapy, breast cancer subtypes, and survival after long-term clinical follow-up

Author

Sherry X. Yang and Eric C. Polley

Subjects

0301 basic medicine, Oncology, Cancer Research, Receptor, ErbB-2, medicine.medical_treatment, Triple Negative Breast Neoplasms, Systemic treatment, Preclinical Study, 0302 clinical medicine, Overall survival, Stage (cooking), skin and connective tissue diseases, Triple-negative breast cancer, Confounding, Middle Aged, Prognosis, Treatment Outcome, Receptors, Estrogen, Chemotherapy, Adjuvant, Hormone receptor, 030220 oncology & carcinogenesis, Immunohistochemistry, Female, Receptors, Progesterone, Adult, medicine.medical_specialty, Breast cancer subtypes, Breast Neoplasms, Disease-Free Survival, 03 medical and health sciences, Breast cancer, HER2, Internal medicine, Biomarkers, Tumor, medicine, Humans, Aged, Hormone receptor (HR), Radiotherapy, business.industry, Cancer, Chemoradiotherapy, Adjuvant, Trastuzumab, medicine.disease, Radiation therapy, 030104 developmental biology, business, Follow-Up Studies

Abstract

Background It remains unclear whether breast cancer subtypes are associated with clinical outcome in patients without any treatment including systemic and radiation therapy as an independent entity. Understanding the survival profiles among subtypes by treatment status could impact optimal selection of treatments. Methods Patients were diagnosed with invasive breast cancer from the community hospitals across four geographical regions of the United States. Expression of hormone receptor (HR) and HER2 in tumor specimens from 1169 patients was centrally determined by immunohistochemistry and fluorescence in situ; breast cancer was classified into HR+/HER2−, HR+/HER2+, triple-negative, and HER2+ subtypes. Overall survival (OS) at a median follow-up of about 15 years among subtypes in untreated patients and those with systemic treatments and radiotherapy was analyzed by Kaplan–Meier method and multivariable analysis adjusting for age, tumor size and grade, number of positive nodes, stage and breast cancer subtypes. Results Without treatment, breast cancer subtypes were not associated with OS (P = 0.983) and remained insignificant for prognosis by multivariable analysis after adjusting for confounders. This contrasted with a significant survival difference across the subtypes in patients with conventional therapies (P

Published

2019

17. Cancer susceptibility gene mutations in type I and II endometrial cancer

Author

Jenna Lilyquist, Sean C. Dowdy, Beverly Long, Chunling Hu, Fergus J. Couch, Eric C. Polley, Jamie N. Bakkum-Gamez, Steven N. Hart, Kun Y. Lee, Amy L. Weaver, and Rohan Gnanaolivu

Subjects

0301 basic medicine, Genes, BRCA2, Genes, BRCA1, Gene mutation, Article, Germline, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, medicine, Humans, Genetic Predisposition to Disease, Gene, Allele frequency, Germ-Line Mutation, Aged, business.industry, Endometrial cancer, Obstetrics and Gynecology, Middle Aged, medicine.disease, Lynch syndrome, Endometrial Neoplasms, Serous fluid, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, Female, business

Abstract

OBJECTIVES: To determine the incidence of germline cancer predisposition gene mutations in patients with endometrial cancer (EC) subtypes. METHODS: Germline DNA was extracted from whole blood collected from consenting patients undergoing primary surgery for EC between 5/2005–11/2016. DNA samples were evaluated by product sequencing from a targeted multiplex PCR panel including 21 known/suspected cancer predisposition genes. Variants were classified as pathogenic/likely pathogenic based on allele frequency (

Published

2019

18. Comparison of the Prevalence of Pathogenic Variants in Cancer Susceptibility Genes in Black Women and Non-Hispanic White Women With Breast Cancer in the United States

Author

Susan M. Domchek, Steven N. Hart, Julie R. Palmer, Katherine L. Nathanson, Christine B. Ambrosone, Fei Chen, Fergus J. Couch, David E. Goldgar, Song Yao, Christopher A. Haiman, Eric C. Polley, and Chunling Hu

Subjects

Cancer Research, medicine.medical_specialty, Population, Breast Neoplasms, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Internal medicine, medicine, Prevalence, Humans, 030212 general & internal medicine, Genetic Testing, Family history, education, CHEK2, Genetic testing, education.field_of_study, White (horse), medicine.diagnostic_test, business.industry, Brief Report, Cancer, Ecological study, Middle Aged, medicine.disease, United States, Oncology, 030220 oncology & carcinogenesis, Case-Control Studies, Female, business

Abstract

IMPORTANCE: The prevalence of germline pathogenic variants (PVs) in cancer susceptibility genes in US Black women compared with non-Hispanic White women with breast cancer is poorly described. OBJECTIVE: To determine whether US Black and non-Hispanic White women with breast cancer have a different prevalence of PVs in 12 cancer susceptibility genes. DESIGN, SETTING, AND PARTICIPANTS: Multicenter, population-based studies in the Cancer Risk Estimates Related to Susceptibility (CARRIERS) consortium. Participants were Black and non-Hispanic White women diagnosed with breast cancer, unselected for family history or age at diagnosis. Data were collected from June 1993 to June 2020; data analysis was performed between September 2020 and February 2021. MAIN OUTCOMES AND MEASURES: Prevalence of germline PVs in 12 established breast cancer susceptibility genes. RESULTS: Among 3946 Black women (mean [SD] age at diagnosis, 56.5 [12.02] y) and 25 287 non-Hispanic White women (mean [SD] age at diagnosis, 62.7 [11.14] y) with breast cancer, there was no statistically significant difference by race in the combined prevalence of PVs in the 12 breast cancer susceptibility genes evaluated (5.65% in Black vs 5.06% in non-Hispanic White women; P = .12). The prevalence of PVs in CHEK2 was higher in non-Hispanic White than Black patients (1.29% vs 0.38%; P

Published

2021

19. Mutations in BRCA1/2 and Other Panel Genes in Patients With Metastatic Breast Cancer —Association With Patient and Disease Characteristics and Effect on Prognosis

Author

Arif B. Ekici, Michael Untch, Matthias Rübner, Steven N. Hart, Matthias W. Beckmann, Kun Y. Lee, Volkmar Müller, Bernhard Volz, Erik Belleville, Markus Wallwiener, Tanja Fehm, Pauline Wimberger, Friedrich Overkamp, Chunling Hu, Diana Lüftner, Peter A. Fasching, Peyman Hadji, Sabrina Uhrig, Arndt Hartmann, Hans Christian Kolberg, Marius Wunderle, Diethelm Wallwiener, Andreas Schneeweiss, Wolfgang Janni, Hans Tesch, Florin Andrei Taran, André Reis, Fergus J. Couch, Sara Y. Brucker, Rohan Gnanaolivu, Siddhartha Yadav, Michael P. Lux, Johannes Ettl, Lothar Häberle, Andreas D. Hartkopf, H Hübner, and Eric C. Polley

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Genes, BRCA2, MEDLINE, Genes, BRCA1, Breast Neoplasms, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Text mining, Internal medicine, medicine, Humans, Clinical significance, In patient, Neoplasm Metastasis, skin and connective tissue diseases, Gene, 030219 obstetrics & reproductive medicine, business.industry, ORIGINAL REPORTS, Middle Aged, medicine.disease, Prognosis, Metastatic breast cancer, 030220 oncology & carcinogenesis, Mutation, Disease characteristics, Female, business

Abstract

PURPOSE Among patients with metastatic breast cancer (mBC), the frequency of germline mutations in cancer susceptibility genes and the clinical relevance of these mutations are unclear. In this study, a prospective cohort of patients with mBC was used to determine mutation rates for breast cancer (BC) predisposition genes, to evaluate the clinical characteristics of patients with mutations, and to assess the influence of mutations on patient outcome. PATIENTS AND METHODS Germline DNA from 2,595 patients with mBC enrolled in the prospective PRAEGNANT registry was evaluated for mutations in cancer predisposition genes. The frequencies of mutations in known BC predisposition genes were compared with results from a prospective registry of patients with nonmetastatic BC sequenced using the same QIAseq method and with public reference controls. Associations between mutation status and tumor characteristics, progression-free survival, and overall survival were assessed. RESULTS Germline mutations in 12 established BC predisposition genes (including BRCA1 and BRCA2) were detected in 271 (10.4%) patients. A mutation in BRCA1 or BRCA2 was seen in 129 patients (5.0%). BRCA1 mutation carriers had a higher proportion of brain metastasis (27.1%) compared with nonmutation carriers (12.8%). Mutations were significantly enriched in PRAEGNANT patients with mBC compared with patients with nonmetastatic BC (10.4% v 6.6%, P < .01). Mutations did not significantly modify progression-free survival or overall survival for patients with mBC. CONCLUSION Multigene panel testing may be considered in all patients with mBC because of the high frequency of germline mutations in BRCA1/2 and other BC predisposition genes. Although the prognosis of mutation carriers and nonmutation carriers with mBC was similar, differences observed in tumor characteristics have implications for treatment and for future studies of targeted therapies.

Published

2021

20. Molecular Profiling-Based Assignment of Cancer Therapy (NCI-MPACT): A Randomized Multicenter Phase II Trial

Author

Nancy Moore, James H. Doroshow, Saiama N. Waqar, Christina L. Rosenberger, Mel Simpson, Richard Piekarz, Alida Palmisano, Funda Meric-Bernstam, Stephen Leong, Yingdong Zhao, P. Mickey Williams, Kanwal Pratap Singh Raghav, Richard Simon, Biswajit Das, S. Kummar, Larry Rubinstein, Chris Karlovich, David J. Sims, Mariam M. Konaté, Ming Chung Li, Eric C. Polley, Jared C. Foster, Alice P. Chen, Geraldine O'Sullivan Coyne, and Chih Jian Lih

Subjects

Adult, Male, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Pyridones, Cancer therapy, Antineoplastic Agents, Pyrimidinones, DNA sequencing, Carboplatin, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Double-Blind Method, Neoplasms, Internal medicine, Temozolomide, medicine, Humans, Everolimus, Aged, Aged, 80 and over, business.industry, Gene Expression Profiling, DNA, Neoplasm, ORIGINAL REPORTS, Targeted Drug Therapy, Middle Aged, Refractory cancer, 030104 developmental biology, Molecular Diagnostic Techniques, 030220 oncology & carcinogenesis, Pyrazoles, Benzimidazoles, Female, business

Abstract

PURPOSEThis trial assessed the utility of applying tumor DNA sequencing to treatment selection for patients with advanced, refractory cancer and somatic mutations in one of four signaling pathways by comparing the efficacy of four study regimens that were either matched to the patient's aberrant pathway (experimental arm) or not matched to that pathway (control arm).MATERIALS AND METHODSAdult patients with an actionable mutation of interest were randomly assigned 2:1 to receive either (1) a study regimen identified to target the aberrant pathway found in their tumor (veliparib with temozolomide or adavosertib with carboplatin [DNA repair pathway], everolimus [PI3K pathway], or trametinib [RAS/RAF/MEK pathway]), or (2) one of the same four regimens, but chosen from among those not targeting that pathway.RESULTSAmong 49 patients treated in the experimental arm, the objective response rate was 2% (95% CI, 0% to 10.9%). One of 20 patients (5%) in the experimental trametinib cohort had a partial response. There were no responses in the other cohorts. Although patients and physicians were blinded to the sequencing and random assignment results, a higher pretreatment dropout rate was observed in the control arm (22%) compared with the experimental arm (6%; P = .038), suggesting that some patients may have had prior tumor mutation profiling performed that led to a lack of participation in the control arm.CONCLUSIONFurther investigation, better annotation of predictive biomarkers, and the development of more effective agents are necessary to inform treatment decisions in an era of precision cancer medicine. Increasing prevalence of tumor mutation profiling and preference for targeted therapy make it difficult to use a randomized phase II design to evaluate targeted therapy efficacy in an advanced disease setting.

Published

2021

21. Pathogenic Variants in Cancer Predisposition Genes and Prostate Cancer Risk in Men of African Ancestry

Author

Kun Y. Lee, Chunling Hu, Kuteesa Job, Jenna Lilyquist, Steven N. Hart, Nicholas J. Boddicker, Sue A. Ingles, Eric C. Polley, Christopher A. Haiman, Lucy Xia, Raed Samara, Xin Sheng, Henry M. Dabanja, Lynne R. Wilkens, George Mutema, Benon Masaba, Loic Le Marchand, Rohan Gnanaolivu, Alexander Lubmawa, Dan Namuguzi, Marco Matejcic, David V. Conti, Stephen Watya, Yesha Patel, Siddhartha Yadav, Vicky Kiddu, and Fergus J. Couch

Subjects

0301 basic medicine, Prostate cancer risk, Oncology, Cancer Research, medicine.medical_specialty, Cancer predisposition, business.industry, DNA Repair Pathway, medicine.disease, Article, 03 medical and health sciences, Prostate cancer, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Internal medicine, medicine, business, Gene

Abstract

PURPOSE In studies of men of European ancestry, rare pathogenic variants in DNA repair pathway genes have been shown to be associated with risk of aggressive prostate cancer. The contribution of rare coding variation to prostate cancer risk in men of African ancestry has not been established. METHODS We sequenced a panel of 19 DNA repair and cancer predisposition genes in 2,453 African American and 1,151 Ugandan cases and controls with prostate cancer. Rare variants were classified as pathogenic or putatively functionally disruptive and examined in association with prostate cancer risk and disease aggressiveness in gene and pathway-level association analyses. RESULTS Pathogenic variants were found in 75 of 2,098 cases (3.6%) and 31 of 1,481 controls (2.1%; odds ratio [OR], 1.82; 95% CI, 1.19 to 2.79; P = .0044), with the association being stronger for more aggressive disease phenotypes (OR, 3.10; 95% CI, 1.54 to 6.23; P = .0022). The highest risks for aggressive disease were observed with pathogenic variants in the ATM, BRCA2, PALB2, and NBN genes, with ORs ranging from approximately 4 to 15 in the combined study sample of African American and Ugandan men. Rare, nonpathogenic, nonsynonymous variants did not have a major impact on risk of overall prostate cancer or disease aggressiveness. CONCLUSION Rare pathogenic variants in DNA repair genes have appreciable effects on risk of aggressive prostate cancer in men of African ancestry. These findings have potential implications for panel testing and risk stratification in this high-risk population.

Published

2020

22. The Contribution of Germline Predisposition Gene Mutations to Clinical Subtypes of Invasive Breast Cancer From a Clinical Genetic Testing Cohort

Author

Jill S. Dolinsky, Fergus J. Couch, Holly LaDuca, David E. Goldgar, Jenna Lilyquist, Swati Shah, Chunling Hu, Hermela Shimelis, Steven N. Hart, Tina Pesaran, Eric C. Polley, Jie Na, and Siddhartha Yadav

Subjects

Adult, Cancer Research, Adolescent, Genotype, Estrogen receptor, Breast Neoplasms, Gene mutation, Cohort Studies, 03 medical and health sciences, Genetic Heterogeneity, Young Adult, 0302 clinical medicine, Breast cancer, Germline mutation, Medicine, Humans, Genetic Predisposition to Disease, Neoplasm Invasiveness, Genetic Testing, skin and connective tissue diseases, CHEK2, Genetic Association Studies, Germ-Line Mutation, 030304 developmental biology, 0303 health sciences, BARD1 Gene, business.industry, Carcinoma, Ductal, Breast, Cancer, Articles, Middle Aged, medicine.disease, United States, Oncology, 030220 oncology & carcinogenesis, Cancer research, Female, business, Ovarian cancer, AcademicSubjects/MED00010

Abstract

Background The germline cancer predisposition genes associated with increased risk of each clinical subtype of breast cancer, defined by estrogen receptor (ER), progesterone receptor (PR), and HER2, are not well defined. Methods A total of 54 555 invasive breast cancer patients with 56 480 breast tumors were subjected to clinical hereditary cancer multigene panel testing. Heterogeneity for predisposition genes across clinical breast cancer subtypes was assessed by comparing mutation frequencies by gene among tumor subtypes and by association studies between each tumor subtype and reference controls. Results Mutations in 15 cancer predisposition genes were detected in 8.6% of patients with ER+/HER2-; 8.9% with ER+/HER2+; 7.7% with ER-/HER2+; and 14.4% of ER-/PR-/HER2- tumors. BRCA1, BRCA2, BARD1, and PALB2 mutations were enriched in ER- and HER2- tumors; RAD51C and RAD51D mutations were enriched in ER- tumors only; TP53 mutations were enriched in HER2+ tumors, and ATM and CHEK2 mutations were enriched in both ER+ and/or HER2+ tumors. All genes were associated with moderate (odds ratio > 2.00) or strong (odds ratio > 5.00) risks of at least one subtype of breast cancer in case-control analyses. Mutations in ATM, BARD1, BRCA1, BRCA2, CHEK2, PALB2, RAD51C, RAD51D, and TP53 had predicted lifetime absolute risks of at least 20.0% for breast cancer. Conclusions Germline mutations in hereditary cancer panel genes confer subtype-specific risks of breast cancer. Combined tumor subtype, age at breast cancer diagnosis, and family history of breast and/or ovarian cancer information provides refined categorical estimates of mutation prevalence for women considering genetic testing.

Published

2020

23. Combined associations of a polygenic risk score and classical risk factors with breast cancer risk

Author

Diether Lambrechts, James Y. Dai, Pascal Guénel, Graham G. Giles, Montserrat Garcia-Closas, Javier Benitez, Thomas Brüning, Georgia Chenevix-Trench, Stig E. Bojesen, Rodney J Scott, Angela Cox, Anthony Howell, Nilanjan Chatterjee, Volker Arndt, Christopher J. Scott, Rudolf Kaaks, A. Heather Eliassen, Clarice R. Weinberg, Kyriaki Michailidou, Melissa C. Southey, Joe Dennis, Xiaoliang Wang, Niclas Håkansson, Anthony J Swerdlow, Laura E. Beane Freeman, Peter A. Fasching, David J. Hunter, Kristan J. Aronson, Jack A. Taylor, Thomas U. Ahearn, Håkan Olsson, Hoda Anton-Culver, Matthias W. Beckmann, Jenny Chang-Claude, Qiuyin Cai, Renske Keeman, Roger L. Milne, Bernd Holleczek, Jolanta Lissowska, Mia M. Gaudet, Paul D.P. Pharoah, Federico Canzian, Andrew F Olshan, Janet E. Olson, Susan M. Gapstur, Amber N Wilcox, John J. Spinelli, Christine L. Clarke, Stella Koutros, Ann Smeets, Brian D. Carter, Tabea Maurer, W Willett, Catriona McLean, Caroline Weltens, Hiltrud Brauch, Arif B. Ekici, Lin Fritschi, Maria Elena Martinez, Nick Orr, Dale P. Sandler, Yon-Dschun Ko, Simon S. Cross, Xiaohong R. Yang, Aaron D. Norman, Zomoroda Abu-Ful, Flavio Lejbkowicz, Per Hall, Allison W. Kurian, Ben Schöttker, Douglas F. Easton, Lothar Haeberle, Hermann Brenner, Manuela Gago-Dominguez, Robert J. MacInnis, Xiao-Ou Shu, Eunjung Lee, Martha S. Linet, kConFab, Aocs Investigators, Sigrid Hatse, Paul L. Auer, Christobel Saunders, Sara Lindström, Jonine D. Figueroa, Melissa A Troester, Parichoy Pal Choudhury, Ana Llaneza, Peter Kraft, Angel Carracedo, Christopher A. Haiman, Jose E. Castelao, Manjeet K. Bolla, Heiko Becher, Fredrick R. Schumacher, Alicia Beeghly-Fadiel, Hedy S. Rennert, Argyrios Ziogas, Charles M. Perou, Leslie Bernstein, Anna González-Neira, Irene L. Andrulis, H. Shelton Earp, Cari M. Kitahara, G Pita, Stacey J Winham, Wei Zheng, Pooja Middha Kapoor, Abctb Investigators, Kathryn J Ruddy, Minouk J. Schoemaker, Robert N. Hoover, Fergus J. Couch, Ute Hamann, Chi Gao, Rulla M. Tamimi, Kamila Czene, D. Gareth Evans, John L. Hopper, Audrey Y. Jung, Loic Le Marchand, Michael Jones, Marike Gabrielson, Celine M. Vachon, Ross L. Prentice, Katie M. O'Brien, Esther M. John, Jennifer Stone, Daniele Campa, Elke M. van Veen, Qin Wang, Jane Heyworth, Alison M. Dunning, William G. Newman, Nasim Mavaddat, Marjanka K. Schmidt, Gad Rennert, Mikael Eriksson, Sabine Behrens, Susan L. Neuhausen, Stephen J. Chanock, Alicja Wolk, and Eric C Polley

Subjects

Cancer Research, Epidemiology, Gene-environment interactions, Logistic regression, Body Mass Index, 0302 clinical medicine, Breast cancer, Medicine, 10. No inequality, Medical History Taking, Estrogen Receptor Status, Aged, 80 and over, 0303 health sciences, Middle Aged, Risk prediction, 3. Good health, Oncology, Receptors, Estrogen, 030220 oncology & carcinogenesis, Female, AcademicSubjects/MED00010, Medical Genetics, medicine.medical_specialty, Breast Neoplasms, Brief Communication, Polymorphism, Single Nucleotide, White People, Genetic susceptibility, Polygenic risk score, Risk factors, 03 medical and health sciences, SDG 3 - Good Health and Well-being, Humans, Genetic Predisposition to Disease, Risk factor, Medicinsk genetik, 030304 developmental biology, Aged, Cancer och onkologi, business.industry, Case-control study, Cancer, Odds ratio, medicine.disease, Logistic Models, Cancer and Oncology, Case-Control Studies, business, Demography

Abstract

We evaluated the joint associations between a new 313-variant PRS (PRS313) and questionnaire-based breast cancer risk factors for women of European ancestry, using 72 284 cases and 80 354 controls from the Breast Cancer Association Consortium. Interactions were evaluated using standard logistic regression and a newly developed case-only method for breast cancer risk overall and by estrogen receptor status. After accounting for multiple testing, we did not find evidence that per-standard deviation PRS313 odds ratio differed across strata defined by individual risk factors. Goodness-of-fit tests did not reject the assumption of a multiplicative model between PRS313 and each risk factor. Variation in projected absolute lifetime risk of breast cancer associated with classical risk factors was greater for women with higher genetic risk (PRS313 and family history) and, on average, 17.5% higher in the highest vs lowest deciles of genetic risk. These findings have implications for risk prevention for women at increased risk of breast cancer. ispartof: JNCI-JOURNAL OF THE NATIONAL CANCER INSTITUTE vol:113 issue:3 pages:329-337 ispartof: location:United States status: published

Published

2020

24. Abstract P6-09-02: Associations between hereditary cancer panel predisposition genes and breast cancer histological subtypes

Author

Fergus J. Couch, David E. Goldgar, Jenna Lilyquist, Eric C. Polley, Jill S. Dolinsky, Steven N. Hart, Chunling Hu, Holly LaDuca, B Tippin-Davis, Tina Pesaran, and Jie Na

Subjects

Oncology, Cancer Research, medicine.medical_specialty, medicine.diagnostic_test, medicine.drug_class, business.industry, PALB2, Cancer, Odds ratio, medicine.disease, Breast cancer, Estrogen, Internal medicine, medicine, Family history, skin and connective tissue diseases, business, Exome, Genetic testing

Abstract

Background: Clinical panel testing has become routine practice for patients that are diagnosed with breast cancer at a young age and/or have a personal or family history of cancer. Associations with known breast cancer genes and breast cancer subtypes have been previously identified, such as BRCA1 associations with estrogen receptor negative (ER-) and triple negative (ER-/PR-/HER2-) breast cancers. However, the cancer predisposition genes associated with each of the four clinical subtypes of breast cancer have not been fully defined. We evaluated 24,901 Caucasian female breast cancer cases receiving clinical panel testing for 23 cancer predisposition genes and assessed associations between mutations in each gene and breast cancer subtypes. Methods: Germline hereditary cancer multigene panel testing results for cancer predisposition genes were obtained for 24,901 Caucasian female breast cancer cases evaluated by a clinical testing laboratory. Information on tumor histology, personal and family history of cancer, age at diagnosis, and previous genetic testing was provided by clinical care providers of patients receiving clinical cancer genetic testing. Breast cancer cases were classified into clinical breast cancer subtypes based on estrogen/progesterone hormone receptor status (HR) and HER2 status: Luminal A (HR+/HER2-), Luminal B (HR+/HER2-), HER2 subtype (HR-/HER2+), and Triple Negative (HR-/HER2-). The frequency of pathogenic or likely pathogenic mutations observed in each subtype was compared against the Exome Aggregation Consortium (ExAC) non-TCGA non-Finnish European population to estimate risks. Results: ATM was associated with moderate risks (odds ratio (OR)>2.0) of Luminal A, Luminal B, and HER2 subtypes of breast cancer, but was not associated with the Triple Negative subtype. PALB2 was associated with moderate risk for Luminal B subtype, but high risk (OR>5.0) for Luminal A, HER2, and triple negative subtypes. TP53 was associated with high risks for Luminal B and HER2 tumors. NBN, MRE11A, and RAD50 were not associated with any subtype of breast cancer. Conclusions: Identifying associations between inherited mutations (odds ratio (OR)>2.0) and breast cancer subtypes can inform clinical risk management, treatment options, and therapeutic development efforts. Citation Format: Lilyquist J, Laduca H, Hu C, Na J, Polley EC, Hart SN, Pesaran T, Tippin-Davis B, Goldgar DE, Dolinsky JS, Couch FJ. Associations between hereditary cancer panel predisposition genes and breast cancer histological subtypes [abstract]. In: Proceedings of the 2017 San Antonio Breast Cancer Symposium; 2017 Dec 5-9; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2018;78(4 Suppl):Abstract nr P6-09-02.

Published

2018

25. The National Cancer Institute ALMANAC: A Comprehensive Screening Resource for the Detection of Anticancer Drug Pairs with Enhanced Therapeutic Activity

Author

Richard F. Camalier, Jeevan P Govindharajulu, Larry Rubinstein, Apurva K. Srivastava, Lawrence W. Anderson, Jerry M. Collins, James H. Doroshow, Melinda G. Hollingshead, Susan Holbeck, James A. Crowell, Eric C. Polley, and Deborah Wilsker

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Drug resistance, Pharmacology, Article, Small Molecule Libraries, Mice, 03 medical and health sciences, chemistry.chemical_compound, In vivo, Cell Line, Tumor, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Animals, Humans, Clofarabine, Bortezomib, business.industry, Cancer, medicine.disease, Xenograft Model Antitumor Assays, National Cancer Institute (U.S.), United States, Clinical trial, 030104 developmental biology, Paclitaxel, chemistry, Nilotinib, Drug Screening Assays, Antitumor, business, medicine.drug

Abstract

To date, over 100 small-molecule oncology drugs have been approved by the FDA. Because of the inherent heterogeneity of tumors, these small molecules are often administered in combination to prevent emergence of resistant cell subpopulations. Therefore, new combination strategies to overcome drug resistance in patients with advanced cancer are needed. In this study, we performed a systematic evaluation of the therapeutic activity of over 5,000 pairs of FDA-approved cancer drugs against a panel of 60 well-characterized human tumor cell lines (NCI-60) to uncover combinations with greater than additive growth-inhibitory activity. Screening results were compiled into a database, termed the NCI-ALMANAC (A Large Matrix of Anti-Neoplastic Agent Combinations), publicly available at https://dtp.cancer.gov/ncialmanac. Subsequent in vivo experiments in mouse xenograft models of human cancer confirmed combinations with greater than single-agent efficacy. Concomitant detection of mechanistic biomarkers for these combinations in vivo supported the initiation of two phase I clinical trials at the NCI to evaluate clofarabine with bortezomib and nilotinib with paclitaxel in patients with advanced cancer. Consequently, the hypothesis-generating NCI-ALMANAC web-based resource has demonstrated value in identifying promising combinations of approved drugs with potent anticancer activity for further mechanistic study and translation to clinical trials. Cancer Res; 77(13); 3564–76. ©2017 AACR.

Published

2017

26. Clinical Activity of the γ-Secretase Inhibitor PF-03084014 in Adults With Desmoid Tumors (Aggressive Fibromatosis)

Author

Shivaani Kummar, Baris Turkbey, Robert S. Meehan, Rasa Vilimas, Peter L. Choyke, Lamin Juwara, Ann Lih, James H. Doroshow, Sandra A. Mitchell, Geraldine O.Sullivan Coyne, Yvonne Horneffer, Alice P. Chen, Eric C. Polley, Amul Choudhary, Paul S. Meltzer, Khanh T. Do, and Lee J. Helman

Subjects

Adult, Male, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Genotype, Tetrahydronaphthalenes, Adenomatous Polyposis Coli Protein, Antineoplastic Agents, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Refractory, Internal medicine, Original Reports, medicine, Humans, Patient Reported Outcome Measures, Young adult, Response Evaluation Criteria in Solid Tumors, beta Catenin, Aged, medicine.diagnostic_test, business.industry, Fibromatosis, Valine, Magnetic resonance imaging, Middle Aged, medicine.disease, Magnetic Resonance Imaging, Surgery, Clinical trial, Fibromatosis, Aggressive, 030104 developmental biology, 030220 oncology & carcinogenesis, Mutation, Retreatment, Aggressive fibromatosis, Female, Amyloid Precursor Protein Secretases, Symptom Assessment, Tomography, X-Ray Computed, business

Abstract

Purpose Desmoid tumors (aggressive fibromatosis) arise from connective tissue cells or fibroblasts. In general, they are slow growing and do not metastasize; however, locally aggressive desmoid tumors can cause severe morbidity and loss of function. Disease recurrence after surgery and/or radiation and diagnosis of multifocal desmoid tumors highlight the need to develop effective systemic treatments for this disease. In this study, we evaluate objective response rate after therapy with the γ-secretase inhibitor PF-03084014 in patients with recurrent, refractory, progressive desmoid tumors. Patients and Methods Seventeen patients with desmoid tumors received PF-03084014 150 mg orally twice a day in 3-week cycles. Response to treatment was evaluated at cycle 1 and every six cycles, that is, 18 weeks, by RECIST (Response Evaluation Criteria in Solid Tumors) version 1.1. Patient-reported outcomes were measured at baseline and at every restaging visit by using the MD Anderson Symptoms Inventory. Archival tumor and blood samples were genotyped for somatic and germline mutations in APC and CTNNB1. Results Of 17 patients accrued to the study, 15 had mutations in APC or CTNNB1 genes. Sixteen patients (94%) were evaluable for response; five (29%) experienced a confirmed partial response and have been on study for more than 2 years. Another five patients with prolonged stable disease as their best response remain on study. Patient-reported outcomes confirmed clinician reporting that the investigational agent was well tolerated and, in subgroup analyses, participants who demonstrated partial response also experienced clinically meaningful and statistically significant improvements in symptom burden. Conclusion PF-03084014 was well tolerated and demonstrated promising clinical benefit in patients with refractory, progressive desmoid tumors who receive long-term treatment.

Published

2017

27. Abstract P5-09-03: Associations between breast cancer subtypes and mutations in cancer predisposition genes identified by clinical genetic testing of breast cancer patients

Author

Jenna Lilyquist, Jill S. Dolinsky, Rachel McFarland, David E. Goldgar, Chunling Hu, Holly LaDuca, Eric C. Polley, Margaret Akinhanmi, Hermela Shimelis, Fergus J. Couch, and Jie Na

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Family Cancer History, business.industry, Cancer, Estrogen receptor, medicine.disease, Breast cancer, Germline mutation, Internal medicine, Epidemiology of cancer, medicine, Cancer research, skin and connective tissue diseases, Ovarian cancer, business, CHEK2

Abstract

Clinical genetic testing of individuals with a personal or family history of breast and ovarian cancer using panels for BRCA1/2 and other candidate cancer predisposition genes has become routine clinical practice. Several of the genes on hereditary cancer testing panels have been strongly associated with specific subtypes of breast cancer. In particular, individuals with germline mutations in BRCA1 predominantly develop estrogen receptor (ER)-negative and triple negative (TN) (estrogen receptor negative, progesterone receptor negative, HER2 negative) breast tumors. In contrast, CHEK2 and ATM mutations have been associated with ER-positive breast cancer. In this study, associations between mutations in panel genes and breast cancer subtypes were evaluated. A cohort of 60,000 breast cancer patients tested for germline cancer predisposing mutations using hereditary cancer gene panels was utilized. Information on personal and family cancer history, age of diagnosis, tumor pathology, and ethnicity of patients was obtained from test requisition forms or by follow up with ordering health care providers. Mutations in each gene were combined into four histological subtypes (triple negative; HER2 positive; ER-positive,HER2-positive; and ER-positive,HER2 negative). Associations for each subtype were estimated by case-control analyses comparing the frequencies of pathogenic mutations in each subtype with frequencies from non-TCGA controls from the Exome Aggregation Consortium (ExAC) database. In addition, case-case analyses were conducted to assess enrichment of gene mutations in specific breast cancer subtypes. Among the observed associations between genes and breast cancer subtypes, mutations in CHEK2 and ATM were highly enriched in luminal breast cancers and BARD1 was specifically associated with TN breast cancer. Refining the spectrum of pathological correlates with mutations in hereditary breast cancer genes will aid gene specific cancer risk management, and may accelerate the development of novel gene-specific therapeutic interventions. Citation Format: Couch FJ, Lilyquist J, Na J, Hu C, Polley EC, Shimelis H, Akinhanmi M, McFarland R, LaDuca H, Goldgar DE, Dolinsky JS. Associations between breast cancer subtypes and mutations in cancer predisposition genes identified by clinical genetic testing of breast cancer patients [abstract]. In: Proceedings of the 2016 San Antonio Breast Cancer Symposium; 2016 Dec 6-10; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2017;77(4 Suppl):Abstract nr P5-09-03.

Published

2017

28. Contribution of Inherited DNA-Repair Gene Mutations to Hormone-Sensitive and Castrate-Resistant Metastatic Prostate Cancer and Implications for Clinical Outcome

Author

David W. Hillman, Siddhartha Yadav, Kun Y. Lee, Steven N. Hart, Manish Kohli, Jie Na, Eric C. Polley, Fergus J. Couch, Rohan Gnanaolivu, and Chunling Hu

Subjects

0301 basic medicine, Cancer Research, DNA repair, business.industry, medicine.disease, Hormone-sensitive, 03 medical and health sciences, Prostate cancer, 030104 developmental biology, 0302 clinical medicine, Castrate resistant, Germline mutation, Oncology, 030220 oncology & carcinogenesis, medicine, Cancer research, Original Report, business

Abstract

PURPOSE To compare the prevalence of germline mutations in metastatic hormone-sensitive prostate cancer (mHSPC) and metastatic castrate-resistant prostate cancer (mCRPC) and assess the impact of mutations on progression to castration resistance and overall survival. METHODS Targeted sequencing of germline DNA from 704 men (221 at the time of mHSPC and 483 at the time of mCRPC) enrolled in two advanced prostate cancer registries at Mayo Clinic between 2003 and 2013 was performed for 21 predisposition genes. Frequencies of pathogenic mutations were compared in patients and reference controls to identify genes enriched in metastatic prostate cancer. Multivariable Cox proportional hazards regression was used to identify predictors of progression to mCRPC and overall survival. RESULTS Sixty-eight germline mutations in 12 genes were identified in 66 men (9.4%). Mutations in ATM, BRCA2, CHEK2, FANCM, and TP53 were significantly enriched (odds ratio greater than 2.0) in the metastatic cohorts compared with reference controls. The frequency of germline mutations was similar for patients with mHSPC and mCRPC (11.8% v 8.3%; P = .16). The median time to progression from mHSPC to mCRPC was 23.1 and 32.5 months for patients with and without mutations, respectively ( P = .96). Although older age at diagnosis, Gleason score greater than 7, elevated alkaline phosphatase level, and high volume of disease were associated with shorter duration of progression to mCRPC and poor overall survival, mutation status was not (progression to mCRPC hazard ratio, 0.81; 95% CI, 0.61 to 1.09; P = .17; overall survival hazard ratio, 1.00; 95% CI, 0.75 to 1.34; P = .98). CONCLUSION Similarly elevated rates of germline predisposition gene mutations in mHSPC and mCRPC suggest that germline genetic testing may help to guide medical management for all patients with advanced metastatic prostate cancer. Mutation status was not associated with shorter progression to mCRPC or poor overall survival.

Published

2019

29. Multigene Hereditary Cancer Panels Reveal High-Risk Pancreatic Cancer Susceptibility Genes

Author

Hermela Shimelis, Steven N. Hart, Jill S. Dolinsky, Chunling Hu, Kun Y. Lee, Eric C. Polley, Holly LaDuca, David E. Goldgar, Jenna Lilyquist, Abigail Thomas, Brigette Tippin Davis, Tina Pesaran, Fergus J. Couch, Mary Helen Black, and Jie Na

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, medicine.diagnostic_test, business.industry, PALB2, Gene mutation, medicine.disease, Article, 3. Good health, MSH6, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, MSH2, CDKN2A, 030220 oncology & carcinogenesis, Internal medicine, Pancreatic cancer, medicine, business, Exome, Genetic testing

Abstract

Purpose The relevance of inherited pathogenic mutations in cancer predisposition genes in pancreatic cancer is not well understood. We aimed to assess the characteristics of patients with pancreatic cancer referred for hereditary cancer genetic testing and to estimate the risk of pancreatic cancer associated with mutations in panel-based cancer predisposition genes in this high-risk population. Methods Patients with pancreatic cancer (N = 1,652) were identified from a 140,000-patient cohort undergoing multigene panel testing of predisposition genes between March 2012 and June 2016. Gene-level mutation frequencies relative to Exome Aggregation Consortium and Genome Aggregation Database reference controls were assessed. Results The frequency of germline cancer predisposition gene mutations among patients with pancreatic cancer was 20.73%. Mutations in ATM, BRCA2, CDKN2A, MSH2, MSH6, PALB2, and TP53 were associated with high pancreatic cancer risk (odds ratio, > 5), and mutations in BRCA1 were associated with moderate risk (odds ratio, > 2). In a logistic regression model adjusted for age at diagnosis and family history of cancer, ATM and BRCA2 mutations were associated with personal history of breast or pancreatic cancer, whereas PALB2 mutations were associated with family history of breast or pancreatic cancer. Conclusion These findings provide insight into the spectrum of mutations expected in patients with pancreatic cancer referred for cancer predisposition testing. Mutations in eight genes confer high or moderate risk of pancreatic cancer and may prove useful for risk assessment for pancreatic and other cancers. Family and personal histories of breast cancer are strong predictors of germline mutations.

Published

2019

30. Breast cancer screening for carriers of ATM, CHEK2, and PALB2 pathogenic variants: A comparative modeling analysis

Author

Amy Trentham-Dietz, Clyde Schecter, Cancer Risk Estimates Related to Susceptibility, Fergus J. Couch, Cancer Intervention, Jeanne S. Mandelblatt, Brian L. Sprague, John M. Hampton, Allison W. Kurian, Martin J. Yaffe, Karla Kerlikowske, Oguzhan Alagoz, Peter Kraft, Diana L. Miglioretti, Natasha K. Stout, H. Amarens Geuzinge, Kathryn P. Lowry, Mark E. Robson, Anna N. A. Tosteson, Nicolien T. van Ravesteyn, Eric C. Polley, and Jennifer M. Yeh

Subjects

Oncology, Cancer Research, medicine.medical_specialty, medicine.diagnostic_test, business.industry, PALB2, medicine.disease, Breast cancer screening, Breast cancer, Internal medicine, medicine, skin and connective tissue diseases, business, CHEK2

Abstract

10500 Background: Inherited pathogenic variants in ATM, CHEK2, and PALB2 confer moderate to high risks of breast cancer. The optimal approach to screening in these women has not been established. Methods: We used two simulation models from the Cancer Intervention and Surveillance Modeling Network (CISNET) and data from the Cancer Risk Estimates Related to Susceptibility consortium (CARRIERS) to project lifetime breast cancer incidence and mortality in ATM, CHEK2, and PALB2 carriers. We simulated screening with annual mammography from ages 40-74 alone and with annual magnetic resonance imaging (MRI) starting at ages 40, 35, 30, and 25. Joint and separate mammography and MRI screening performance was based on published literature. Lifetime outcomes per 1,000 women were reported as means and ranges across both models. Results: Estimated risk of breast cancer by age 80 was 22% (21-23%) for ATM, 28% (26-30%) for CHEK2, and 40% (38-42%) for PALB2. Screening with MRI and mammography reduced breast cancer mortality by 52-60% across variants (Table). Compared to no screening, starting MRI at age 30 increased life years (LY)/1000 women by 501 (478-523) in ATM, 620 (587-652) in CHEK2, and 1,025 (998-1,051) in PALB2. Starting MRI at age 25 versus 30 gained 9-12 LY/1000 women with 517-518 additional false positive screens and 197-198 benign biopsies. Conclusions: For women with ATM, CHEK2, and PALB2 pathogenic variants, breast cancer screening with MRI and mammography halves breast cancer mortality. These mortality benefits are similar to those for MRI screening for BRCA1/2 mutation carriers and should inform practice guidelines.[Table: see text]

Published

2021

31. Abstract P5-03-07: Distribution of the 21-gene recurrence score (RS) assay (Oncotype DX) in carriers of germline mutations associated with breast cancer predisposition syndromes

Author

Minetta C. Liu, Roberto A. Leon-Ferre, Eric C. Polley, Matthew P. Goetz, Karthik V. Giridhar, Grace M. Choong, Siddartha Yadav, and Fergus J. Couch

Subjects

Oncology, Cancer Research, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Cancer, medicine.disease, Breast cancer, Germline mutation, MUTYH, CDKN2A, MSH2, Internal medicine, Medicine, business, Oncotype DX, CHEK2

Abstract

Background: BRCA1/2 carriers have higher scores in the 21-gene RS assay compared to non-carriers. Little is known about the 21-gene RS patterns in women harboring germline mutations in genes outside BRCA1/2. Methods: We utilized the Mayo Clinic Breast Cancer Study Registry to identify individuals with non-metastatic estrogen receptor positive breast cancer and clinical 21-gene RS results available. We cross-referenced this with an institutional registry of patients tested for hereditary cancer genes, either from the electronic health record or from a research study conducted using a custom QIAseq multiplex amplicon-based panel (Qiagen). The latter assay covered target regions of all coding regions for the following predisposition genes: ATM, BARD1, BLM, BRCA1, BRCA2, BRIP1, CDH1, CDKN2A, CHEK2, ERCC2, FANCC, FANCM, MLH1, MRE11A, MSH2, MSH6, MUTYH, NBN, NF1, PALB2, PMS2, PTEN, RAD50, RAD51C, RAD51D, RECQL, PRSS1, STK11, TP53, and XRCC2. Student’s t-test was used to compare 21-gene RS between carriers, non-carriers, and specific carrier genes (JMP v 14.0). Results: 282 patients were identified with early stage breast cancer and 21-gene RS available, including 85 known mutation carriers and 197 non-carriers (or unknown carrier status). Germline mutations were identified in CHEK2 (n=25), BRCA2 (n=18), ATM (n=10), BRCA1 (n=5), PALB2 (n=5), TP53 (n=3), FANCM (n=2), MUTYH (n=2), PMS2 (n=2), PPM1D (n=2), RECQL (n=2), BARD1 (n=1), BLM (n=1), CDH1 (n=1), ERCC2 (n=1), FANCC (n=1), MSH6 (n=1), NBN (n=1), PRSS1 (n=1), and PTEN (n=1). In the entire cohort, the mean 21-gene RS was 20.4 in carriers and 18.0 in non-carriers (p=0.11). We performed individual analyses on specific genes identified in ≥ 5 patients (table 1). Compared to the mean RS in non-carriers (18.0), higher mean RS were observed in patients harboring BRCA1 (38.8, p=0.002), PALB2 (26.6, p=0.0724), and BRCA2 (23.2, p=0.0453). The RS in CHEK2 and ATM carriers were comparable to those of non-carriers. Conclusions: We observed differences in RS score distribution based on specific mutated breast cancer predisposition genes. Further validation of the distribution and performance of the 21-gene RS in germline carriers is needed. 21-gene RS scorenMedian RSMean≤1516-25≥26n%n%n%CHEK2251616.61248728624BRCA2182123.2211.11161.1527.8ATM101716.9330550220BRCA153635.8120120360PALB253326.6120120360None1971518.09950.367343115.7 Citation Format: Karthik V Giridhar, Grace M Choong, Siddartha Yadav, Eric C Polley, Roberto A Leon-Ferre, Minetta C Liu, Matthew P Goetz, Fergus J Couch. Distribution of the 21-gene recurrence score (RS) assay (Oncotype DX) in carriers of germline mutations associated with breast cancer predisposition syndromes [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr P5-03-07.

Published

2020

32. Abstract PD3-02: Polygenic risk scores provide clinically meaningful risk stratification among women carrying moderate penetrance pathogenic variants in breast cancer predisposition genes: Results from the CARRIERS study

Author

Katherine L. Nathanson, Fergus J. Couch, Nicholas J. Boddicker, Susan L. Neuhausen, Eric C. Polley, Steven N. Hart, Chi Gao, Song Yao, Christopher A. Haiman, Raed Samara, Jie Na, Kun Y. Lee, David E. Goldgar, Janet E. Olson, Mia Gaudet, Rohan Gnanaolivu, Chunling Hu, Amy Trentham-Dietz, Leslie Bernstein, Susan M. Domchek, Paul W. Auer, Jeffrey N. Weitzel, and Peter Kraft

Subjects

Oncology, Cancer Research, medicine.medical_specialty, education.field_of_study, medicine.diagnostic_test, business.industry, PALB2, Population, Genome-wide association study, medicine.disease, Penetrance, Breast cancer, Internal medicine, medicine, Breast MRI, Family history, skin and connective tissue diseases, education, business, CHEK2

Abstract

Background: Pathogenic variants detected in multi-gene cancer predisposition panels are increasingly used to counsel women regarding their risk for breast cancer. However, the clinical implications of moderate penetrance genes (e.g. CHEK2, ATM) remain unclear. Breast MRI is indicated for women with a lifetime risk of breast cancer of >20%, and polygenic risk scores (PRS) based on common variants discovered in recent genome-wide association studies (GWAS) may identify women with pathogenic variants in CHEK2 and ATM who are above or below this level of risk. PRS may also stratify carriers with substantially elevated lifetime risks of breast cancer. Previous work found that PRS modified breast cancer risk in carriers of pathogenic variant in BRCA1 or BRCA2, but the joint effects of pathogenic variants and PRS have not been studied in samples drawn from the general population. There is also no published study evaluating the effect of PRS among women with pathogenic variants in genes other than BRCA1/2 and CHEK2. Here, we evaluated the joint effects of PRS and pathogenic variants in ten established breast cancer predisposition genes in a population-based case-control sample. Method: We analyzed 43,144 non-Hispanic European-ancestry individuals (20,988 controls and 22,120 cases) drawn from 7 cohorts and 2 population-based case-control studies in the CAnceR RIsk Estimates Related to Susceptibility” (CARRIERS) consortium. Targeted sequencing was performed using a dual bar-coded QIAseq panel of breast cancer predisposition genes. Variant calling was conducted with Haplotype Caller and Vardict. The PRS was calculated based on 106 common variants using effect estimates from the largest published breast cancer GWAS. Genetic status was evaluated for 10 breast cancer predisposition genes: ATM, BARD1, BRCA1, BRCA2, BRIP1, CDH1, CHEK2, NF1, PALB2 and TP53. Lasso Penalized regression was performed to assess the combined effect on overall breast cancer of pathogenic variants and common variants (including main and interaction effects between age, family history, carrier status and PRS). The fraction of women at >2-fold increased risk (which is associated with approximately 20% lifetime risk of breast cancer) was calculated for pathogenic variant carriers and non-carriers of different family history and age groups (70yrs old). Results: Among non-carriers, one standard deviation change in the PRS was associated with a 1.63x change in odds of breast cancer. The best-fitting risk model did not include any PRS-by-carrier interaction terms, implying the relative risk gradient associated with PRS among women with pathogenic variants is similar to that among non-carriers. For carriers of pathogenic variants in moderate penetrance genes with no family history of breast cancer, the PRS can identify 60.6% of ATM pathogenic variant carriers and 30% of CHEK2 pathogenic variant carriers that have less than 2-fold risk of breast cancer; when carriers have a family history of breast cancer, the PRS can identify 30% of ATM pathogenic variant carriers and 11.8% of CHEK2 pathogenic variant carriers with less than 2-fold risk of breast cancer. Conclusion: In our large, population-based case-control study, the effect of the PRS among pathogenic variant carriers was not significantly different than among non-carriers. However, the PRS may be particularly important for estimating breast cancer risk among carriers of pathogenic variants in moderate penetrance genes such as CHEK2 and ATM, enabling a more precise approach for MRI screening strategy and breast cancer risk management. Citation Format: Chi Gao, Eric C. Polley, Chunling Hu, Steven N. Hart, Rohan Gnanaolivu, Kun Y. Lee, Jie Na, Nicholas J. Boddicker, Raed Samara, Paul Auer, Leslie Bernstein, Mia Gaudet, Amy Trentham-Dietz, Song Yao, Christopher Haiman, Janet E. Olson, Susan Neuhausen, Jeffrey N. Weitzel, David E. Goldgar, Susan Domchek, Katherine L. Nathanson, Fergus J. Couch, Peter Kraft, on behalf of the CARRIERS consortium. Polygenic risk scores provide clinically meaningful risk stratification among women carrying moderate penetrance pathogenic variants in breast cancer predisposition genes: Results from the CARRIERS study [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr PD3-02.

Published

2020

33. Abstract PD3-01: Population-based breast cancer risk estimates for predisposition gene mutations: Results from the CARRIERS study

Author

Christine B. Ambrosone, Celine M. Vachon, Josh Klebba, Bruce W. Eckloff, Janet E. Olson, Katherine L. Nathanson, Esther M. John, Chi Gao, Susan L. Neuhausen, Julie R Palmer, Eric C. Polley, Clarice R. Weinberg, Hoda Anton-Culver, Jack A. Taylor, Christopher A. Haiman, Dale P. Sandler, Mia M. Gaudet, David E. Goldgar, Peter Kraft, Rohan Gnanaolivu, Song Yao, Jeffrey N. Weitzel, Nicholas J. Boddicker, Raed Samara, Kun Y. Lee, Steven N. Hart, Susan M. Domchek, Paul L. Auer, Amy Trentham-Dietz, Fergus J. Couch, Jie Na, Tuya Pal, Chunling Hu, and Leslie Bernstein

Subjects

Oncology, Cancer Research, medicine.medical_specialty, education.field_of_study, medicine.diagnostic_test, business.industry, Population, Cancer, Gene mutation, medicine.disease, Breast cancer, Germline mutation, Internal medicine, Cancer screening, Medicine, business, education, CHEK2, Genetic testing

Abstract

Germline mutations in several cancer predisposition genes included in hereditary multigene testing panels have been associated with increased breast cancer risk. However, estimates of breast cancer risks for each gene have in large part been derived from studies of high-risk populations enriched for family history of breast and ovarian cancer, young age of breast cancer diagnosis, or founder mutations. The breast cancer risks associated with mutations in many of these genes in the general population remain to be clearly defined. As clinical hereditary cancer genetic testing is already provided to many women at increased risk and may soon be offered to all breast cancer patients, population-based risk estimates associated with predisposition gene mutations will be needed for appropriate clinical management of mutation carriers. The “CAnceR RIsk Estimates Related to Susceptibility” (CARRIERS) consortium of 17 cohort-based case-control, population-based case-control, and family studies focused on estimation of population-based breast cancer risks and penetrance analysis for mutations in known and candidate breast cancer predisposition genes. Germline DNA from 39486 breast cancer cases and 35868 matched controls was subjected to dual bar-coded QIAseq multiplex amplification of 1733 target regions in 37 predisposition genes. Products from sets of 768 samples were pooled and sequenced in each lane of a HiSeq 4000 system. Mutations were called by GATK Haplotype Caller and Verdict. High quality sequence data was obtained for 99.3% of target regions. Here we report on results from 34741 population-based breast cancer cases and 32728 matched unaffected controls. The mean age of breast cancer diagnosis for cases was 61.2 years and mean age for controls was 61.1 years. Overall, 20.9% of cases and 14.3% of controls had a family history of breast cancer. Furthermore, 74.3% of cases and 75.8% of controls were non-Hispanic white, whereas 13.3% of cases and 15.3% of controls were African American. Among cases with tumor information available, 81.7% were ER-positive and 7.7% were triple negative breast cancers (TNBC). We assessed mutation frequencies in 24 genes including 12 established breast cancer predisposition genes (ATM, BARD1, BRCA1, BRCA2, CDH1, CHEK2, NF1, PALB2, PTEN, RAD51C, RAD51D, andTP53). The overall mutation frequency was 6.2% in cases and 2.7% in controls. Case-control association analysis after adjusting for study, age, family history of breast cancer, and race/ethnicity showed that BRCA1(OR=7.45; 95%CI:5.24-10.95) and BRCA2(OR=5.31; 95%CI:4.15-6.88) were associated with high risks of breast cancer in the general population. However, PALB2mutations were only associated with moderate risks (OR=3.63; 95%CI:2.57-5.26). ATMmutations conferred attenuated risks (OR=1.83; 95%CI:1.47-2.28) relative to studies of high-risk families or young onset breast cancers. NBNmutations were not associated with increased breast cancer risk. Mutations in BARD1, RAD51C, RAD51Dand XRCC2were specifically significantly associated with moderate risks of ER-negative breast cancer and TNBC, whereas mutations in ATM, CDH1and CHEK2were specifically significantly associated with ER-positive disease. On the basis of these findings age-related absolute breast cancer risks for commonly mutated genes were estimated. Overall, results from the CARRIERS study establish that mutations in predisposition genes are associated with lower risks of breast cancer in the general population than in enriched populations including high-risk families and young onset, bilateral, or multiple primary cases. We anticipate that the results from this study will inform cancer screening and other risk management strategies for women in the general population with mutations in predisposition genes. Citation Format: Fergus J Couch, Chunling Hu, Steven N Hart, Rohan Gnanaolivu, Kun Y Lee, Jie Na, Chi Gao, Nicholas J Boddicker, Bruce Eckloff, Raed Samara, Josh Klebba, Christine B Ambrosone, Hoda Anton-Culver, Paul Auer, Leslie Bernstein, Mia M Gaudet, Christopher Haiman, Esther M John, Susan Neuhausen, Janet E Olson, Tuya Pal, Julie R Palmer, Dale P Sandler, Jack A Taylor, Amy Trentham-Dietz, Celine M Vachon, Clarice Weinberg, Song Yao, Jeffrey N Weitzel, David E Goldgar, Susan M Domchek, Katherine L Nathanson, Peter Kraft, Eric C Polley. Population-based breast cancer risk estimates for predisposition gene mutations: Results from the CARRIERS study [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr PD3-01.

Published

2020

34. Triple-negative breast cancer risk genes identified by multigene hereditary cancer panel testing

Author

Margaret Akinhanmi, Brigette Tippin Davis, Priyanka Sharma, Drakoulis Yannoukakos, Eric C. Polley, Raymond Moore, David E. Goldgar, Peter A. Fasching, Jill S. Dolinsky, Abigail Thomas, Heli Nevanlinna, Judy Garber, Diana Eccles, Hiltrud Brauch, Andrew K. Godwin, Bing Jian Feng, Holly LaDuca, Angela Cox, Song Yao, Hermela Shimelis, Jie Na, Florentia Fostira, Steven N. Hart, Fergus J. Couch, Tina Pesaran, Amanda Ewart-Toland, Chunling Hu, Jenna Lilyquist, Irene Konstantopoulou, Doctoral Programme in Biomedicine, Department of Obstetrics and Gynecology, and Clinicum

Subjects

0301 basic medicine, Oncology, Male, Cancer Research, Triple Negative Breast Neoplasms, PHENOTYPE, 0302 clinical medicine, Gene Frequency, Risk Factors, Odds Ratio, CONFER SUSCEPTIBILITY, Age of Onset, Triple-negative breast cancer, medicine.diagnostic_test, WOMEN, Articles, Middle Aged, 3. Good health, 030220 oncology & carcinogenesis, SURVIVAL, Female, Adult, medicine.medical_specialty, PALB2, 3122 Cancers, OVARIAN-CANCER, 03 medical and health sciences, Young Adult, Breast cancer, Internal medicine, medicine, Biomarkers, Tumor, Humans, Genetic Predisposition to Disease, Genetic Testing, INHERITED MUTATIONS, Alleles, Genetic Association Studies, Genetic testing, REPAIR, Cancer prevention, business.industry, Case-control study, Cancer, Odds ratio, medicine.disease, 030104 developmental biology, Case-Control Studies, Mutation, business, Genome-Wide Association Study

Abstract

Background\ud Germline genetic testing with hereditary cancer gene panels can identify women at increased risk of breast cancer. However, those at increased risk of triple-negative (estrogen receptor–negative, progesterone receptor–negative, human epidermal growth factor receptor–negative) breast cancer (TNBC) cannot be identified because predisposition genes for TNBC, other than BRCA1, have not been established. The aim of this study was to define the cancer panel genes associated with increased risk of TNBC.\ud \ud Methods\ud Multigene panel testing for 21 genes in 8753 TNBC patients was performed by a clinical testing laboratory, and testing for 17 genes in 2148 patients was conducted by a Triple Negative Breast Cancer Consortium (TNBCC) of research studies. Associations between deleterious mutations in cancer predisposition genes and TNBC were evaluated using results from TNBC patients and reference controls.\ud \ud Results\ud Germline pathogenic variants in BARD1, BRCA1, BRCA2, PALB2, and RAD51D were associated with high risk (odds ratio > 5.0) of TNBC and greater than 20% lifetime risk for overall breast cancer among Caucasians. Pathogenic variants in BRIP1, RAD51C, and TP53 were associated with moderate risk (odds ratio > 2) of TNBC. Similar trends were observed for the African American population. Pathogenic variants in these TNBC genes were detected in 12.0% (3.7% non-BRCA1/2) of all participants.\ud \ud Conclusions\ud Multigene hereditary cancer panel testing can identify women with elevated risk of TNBC due to mutations in BARD1, BRCA1, BRCA2, PALB2, and RAD51D. These women can potentially benefit from improved screening, risk management, and cancer prevention strategies. Patients with mutations may also benefit from specific targeted therapeutic strategies.

Published

2018

35. The NCI Transcriptional Pharmacodynamics Workbench: A Tool to Examine Dynamic Expression Profiling of Therapeutic Response in the NCI-60 Cell Line Panel

Author

Eric C. Polley, Mariam M. Konaté, Hossein A. Hamed, Yingdong Zhao, Dmitriy Sonkin, James H. Doroshow, Erik Harris, Richard Simon, John Connelly, Anne Monks, Beverly A. Teicher, Melanie A. Simpson, Alida Palmisano, Laura K. Fogli, Ming Chung Li, Jianwen Fang, Curtis Hose, Annamaria Rapisarda, Andrea Regier Voth, Sarah B. Miller, Xiaolin Wu, and Julia Krushkal

Subjects

0301 basic medicine, Therapeutic gene modulation, Drug, Cancer Research, Cell type, media_common.quotation_subject, Antineoplastic Agents, Computational biology, Biology, Deoxycytidine, Article, Translational Research, Biomedical, 03 medical and health sciences, Erlotinib Hydrochloride, 0302 clinical medicine, Cell Line, Tumor, Biomarkers, Tumor, Humans, media_common, Early Growth Response Protein 1, Oligonucleotide Array Sequence Analysis, Internet, Vorinostat, Dose-Response Relationship, Drug, Gene Expression Profiling, Gemcitabine, National Cancer Institute (U.S.), United States, Gene expression profiling, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, Cell culture, 030220 oncology & carcinogenesis, Pharmacodynamics, Cancer cell, Drug Screening Assays, Antitumor, Intracellular, Signal Transduction

Abstract

The intracellular effects and overall efficacies of anticancer therapies can vary significantly by tumor type. To identify patterns of drug-induced gene modulation that occur in different cancer cell types, we measured gene-expression changes across the NCI-60 cell line panel after exposure to 15 anticancer agents. The results were integrated into a combined database and set of interactive analysis tools, designated the NCI Transcriptional Pharmacodynamics Workbench (NCI TPW), that allows exploration of gene-expression modulation by molecular pathway, drug target, and association with drug sensitivity. We identified common transcriptional responses across agents and cell types and uncovered gene-expression changes associated with drug sensitivity. We also demonstrated the value of this tool for investigating clinically relevant molecular hypotheses and identifying candidate biomarkers of drug activity. The NCI TPW, publicly available at https://tpwb.nci.nih.gov, provides a comprehensive resource to facilitate understanding of tumor cell characteristics that define sensitivity to commonly used anticancer drugs. Significance: The NCI Transcriptional Pharmacodynamics Workbench represents the most extensive compilation to date of directly measured longitudinal transcriptional responses to anticancer agents across a thoroughly characterized ensemble of cancer cell lines.

Published

2018

36. Microbiome-TP53 Gene Interaction in Human Lung Cancer

Author

Joshua Chang Mell, Alex M. Valm, Sven Bilke, Curtis C. Harris, Clayton Deming, Sean Conlan, Tricia M. Stickrod, Tomer Cooks, Joshua P. Earl, Amiran Dzutsev, Marina Walther-Antonio, Julie A. Segre, Mohammed Safwan Ali Khan, Jessica Beck, Bríd M. Ryan, Sergey Balashov, K. Leigh Greathouse, Garth D. Ehrlich, Archana S. Bhat, James R. White, Paul S. Meltzer, Eric C. Polley, Elise D. Bowman, Valery Bliskovsky, Julia Oh, Ana I. Robles, Jarosław E. Król, Alexis N. Hokenstad, Marbin Pineda, Ashley J. Vargas, Giorgio Trinchieri, and Natalia von Muhlinen

Subjects

Lung, biology, Acidovorax, Somatic cell, In situ hybridization, biology.organism_classification, medicine.disease, medicine.disease_cause, medicine.anatomical_structure, Gene interaction, medicine, Cancer research, Microbiome, Lung cancer, Carcinogenesis

Abstract

BackgroundLung cancer is the leading cancer diagnosis worldwide and the number one cause of cancer deaths. Exposure to cigarette smoke, the primary risk factor in lung cancer, reduces epithelial barrier integrity and increases susceptibility to infections. Herein, we hypothesized that somatic mutations together with cigarette smoke generate a dysbiotic microbiota that is associated with lung carcinogenesis. Using lung tissue from controls (n=33) and cancer cases (n=143), we conducted 16S rRNA bacterial gene sequencing, with RNA-seq data from lung cancer cases in The Cancer Genome Atlas (n=1112) serving as the validation cohort.ResultsOverall, we demonstrate a lower alpha diversity in normal lung as compared to non-tumor adjacent or tumor tissue. In squamous cell carcinoma (SCC) specifically, a separate group of taxa were identified, in which Acidovorax was enriched in smokers (P =0.0013). Acidovorax temporans was identified by fluorescent in situ hybridization within tumor sections, and confirmed by two separate 16S rRNA strategies. Further, these taxa, including Acidovorax, exhibited higher abundance among the subset of SCC cases with TP53 mutations, an association not seen in adenocarcinomas (AD).ConclusionsThe results of this comprehensive study show both a microbiome-gene and microbiome-exposure interactions in SCC lung cancer tissue. Specifically, tumors harboring TP53 mutations, which can damage epithelial function, have a unique bacterial consortia which is higher in relative abundance in smoking-associated SCC. Given the significant need for clinical diagnostic tools in lung cancer, this study may provide novel biomarkers for early detection.

Published

2018

37. Sarcoma Cell Line Screen of Oncology Drugs and Investigational Agents Identifies Patterns Associated with Gene and microRNA Expression

Author

Beverly A. Teicher, Michael Selby, Rene Delosh, John Connelly, Russell Reinhart, Thomas Silvers, Joel Morris, David Evans, Chad Ogle, Eric C. Polley, Julie Laudeman, Anne Monks, Erik Harris, and Mark Kunkel

Subjects

Adult, Cancer Research, Poly (ADP-Ribose) Polymerase-1, Poly(ADP-ribose) Polymerase Inhibitors, Biology, Article, Receptor, IGF Type 1, Aurora kinase, Aurora Kinases, Cell Line, Tumor, Gene expression, microRNA, medicine, Cluster Analysis, Humans, Child, Protein Kinase Inhibitors, Gene, Oligonucleotide Array Sequence Analysis, Gene Expression Profiling, Sarcoma, Drugs, Investigational, MAP Kinase Kinase Kinases, medicine.disease, Phenotype, Bromodomain, Gene Expression Regulation, Neoplastic, Gene expression profiling, MicroRNAs, Oncology, Cancer research, Drug Screening Assays, Antitumor, Poly(ADP-ribose) Polymerases

Abstract

The diversity in sarcoma phenotype and genotype make treatment of this family of diseases exceptionally challenging. Sixty-three human adult and pediatric sarcoma lines were screened with 100 FDA-approved oncology agents and 345 investigational agents. The investigational agents' library enabled comparison of several compounds targeting the same molecular entity allowing comparison of target specificity and heterogeneity of cell line response. Gene expression was derived from exon array data and microRNA expression was derived from direct digital detection assays. The compounds were screened against each cell line at nine concentrations in triplicate with an exposure time of 96 hours using Alamar blue as the endpoint. Results are presented for inhibitors of the following targets: aurora kinase, IGF-1R, MEK, BET bromodomain, and PARP1. Chemical structures, IC50 heat maps, concentration response curves, gene expression, and miR expression heat maps are presented for selected examples. In addition, two cases of exceptional responders are presented. The drug and compound response, gene expression, and microRNA expression data are publicly available at http://sarcoma.cancer.gov. These data provide a unique resource to the cancer research community. Mol Cancer Ther; 14(11); 2452–62. ©2015 AACR.

Published

2015

38. Risk of Different Cancers Among First-degree Relatives of Pancreatic Cancer Patients: Influence of Probands' Susceptibility Gene Mutation Status

Author

Rohan Gnanaolivu, Ann L. Oberg, Robert R. McWilliams, Eric C. Polley, William R. Bamlet, Hermela Shimelis, Samuel O. Antwi, Kari G. Chaffee, Chunling Hu, Steven N. Hart, Fergus J. Couch, Gloria M. Petersen, Sarah E Fagan, and Jenna Lilyquist

Subjects

Proband, Oncology, Male, Cancer Research, medicine.medical_specialty, 03 medical and health sciences, 0302 clinical medicine, Risk Factors, Pancreatic cancer, Internal medicine, Neoplasms, Epidemiology, medicine, Humans, Family, Genetic Predisposition to Disease, Genetic Testing, Prospective Studies, First-degree relatives, Family history, Germ-Line Mutation, Genetic testing, medicine.diagnostic_test, business.industry, Incidence (epidemiology), Cancer, Articles, Middle Aged, medicine.disease, Prognosis, Pancreatic Neoplasms, 030220 oncology & carcinogenesis, Female, business, Follow-Up Studies

Abstract

BACKGROUND: Increased risk of malignancies other than pancreatic cancer (PC) has been reported among first-degree relatives (FDRs) of PC patients; however, the roles of susceptibility gene mutations are unclear. We assessed risk for 15 cancers among FDRs of unselected PC probands. METHODS: Data on 17 162 FDRs, with more than 336 000 person-years at risk, identified through 2305 sequential PC probands enrolled at Mayo Clinic (2000–2016) were analyzed. Family history data were provided by the probands. Standardized incidence ratios (SIRs) and 95% confidence intervals (CIs) were calculated, comparing malignancies observed among the FDRs with that expected using Surveillance, Epidemiology, and End Results (SEER) data. Genetic testing was performed among a subset of probands (n = 2094), enabling stratified analyses among FDRs based on whether the related proband tested positive or negative for inherited mutation in 22 sequenced cancer susceptibility genes. All statistical tests were two-sided. RESULTS: Compared with SEER, PC risk was twofold higher among FDRs of PC probands (SIR = 2.04, 95% CI = 1.78 to 2.31, P < .001). Primary liver cancer risk was elevated among female FDRs (SIR = 2.10, 95% CI = 1.34 to 3.12, P < .001). PC risk was more elevated among FDRs of mutation-positive probands (SIR = 4.32, 95% CI = 3.10 to 5.86) than FDRs of mutation-negative probands (SIR = 1.77, 95% CI = 1.51 to 2.05, between-group P < .001). FDR PC risk was higher when the related proband was younger than age 60 years at diagnosis and mutation-positive (SIR = 5.24, 95% CI = 2.93 to 8.64) than when the proband was younger than age 60 years but mutation-negative (SIR = 1.76, 95% CI = 1.21 to 2.47, between-group P < .001). Breast (SIR = 1.29, 95% CI = 1.01 to 1.63) and ovarian (SIR = 2.38, 95% CI = 1.30 to 4.00) cancers were elevated among FDRs of mutation-positive probands. CONCLUSIONS: Our study substantiates twofold risk of PC among FDRs of PC patients and suggests increased risk for primary liver cancer among female FDRs. FDRs of susceptibility mutation carriers had substantially increased risk for PC and increased risk for breast and ovarian cancers.

Published

2017

39. Societal challenges of precision medicine: Bringing order to chaos

Author

Augustinus van Dongen, Jeffrey A. Moscow, Nils Wilking, Daniel Hochhauser, Erasmus Schneider, Jonas Bergh, Adrian Senderowicz, Ultan McDermott, Simon J. Dovedi, Philip A. Beer, John W.M. Martens, Robert L. Becker, Mehdi Mesri, Tawnya C. McKee, Shakun Malik, Denis Lacombe, Roberto Salgado, Thomas Lillie, Tracy Lively, Irene Norstedt, Jan Bogaerts, Kathy Oliver, Moritz Gerstung, Francesco Pignatti, Olli Tenhunen, Hartmut Juhl, Helen M. Moore, Stefan Michiels, Richard L. Schilsky, Kim Lyerly Herbert, Antonio Tito Fojo, Robert J. Kinders, Daniel O’Connor, Christine Vietz, Sabine Tejpar, Stephen M. Hewitt, Eric C. Polley, Nitzan Rosenfeld, Jan H.M. Schellens, Sumimasa Nagai, Shyamala Maheswaran, Vassilis Golfinopoulos, Wim J.G. Oyen, and Medical Oncology

Subjects

0301 basic medicine, Cancer Research, business.industry, media_common.quotation_subject, Genomic signature, Routine practice, Precision medicine, Bioinformatics, Article, Clinical trial, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Promotion (rank), Oncology, Risk analysis (engineering), Drug development, Assay validation: biomarkers: Preanalytical and analytical validation: precision oncology, Order (exchange), 030220 oncology & carcinogenesis, Medicine, Biomarker (medicine), business, ta317, media_common

Abstract

The increasing number of drugs targeting specific proteins implicated in tumourigenesis and the commercial promotion of relatively affordable genome-wide analyses has led to an increasing expectation among patients with cancer that they can now receive effective personalised treatment based on the often complex genomic signature of their tumour. For such approaches to work in routine practice, the development of correspondingly complex biomarker assays through an appropriate and rigorous regulatory framework will be required. It is becoming increasingly evident that a re-engineering of clinical research is necessary so that regulatory considerations and procedures facilitate the efficient translation of these required biomarker assays from the discovery setting through to clinical application. This article discusses the practical requirements and challenges of developing such new precision medicine strategies, based on leveraging complex genomic profiles, as discussed at the Innovation and Biomarkers in Cancer Drug Development meeting (8th-9th September 2016, Brussels, Belgium).

Published

2017

40. Interleukin-4 and interleukin-13 increase NADPH oxidase 1-related proliferation of human colon cancer cells

Author

Jiamo Lu, Jennifer L. Meitzler, Smitha Antony, Han Liu, Eric C. Polley, Krishnendu Roy, Yongzhong Wu, Guojian Jiang, Agnes Juhasz, and James H. Doroshow

Subjects

0301 basic medicine, medicine.medical_specialty, Colorectal cancer, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Cell Line, Tumor, medicine, Humans, Neoplastic transformation, Interleukin 4, Cell Proliferation, reactive oxygen species, NADPH oxidase, Interleukin-13, biology, business.industry, GATA3, NADPH Oxidase 1, medicine.disease, Oxidative Stress, 030104 developmental biology, Endocrinology, Oncology, colon cancer, 030220 oncology & carcinogenesis, NOX1, Interleukin 13, Colonic Neoplasms, biology.protein, Cancer research, cardiovascular system, Interleukin-4, business, Priority Research Paper

Abstract

// Han Liu 1 , Smitha Antony 1 , Krishnendu Roy 1 , Agnes Juhasz 2 , Yongzhong Wu 2 , Jiamo Lu 2 , Jennifer L. Meitzler 2 , Guojian Jiang 2 , Eric Polley 1 and James H. Doroshow 1,2 1 Division of Cancer Treatment and Diagnosis, National Cancer Institute, Bethesda, Maryland, USA 2 The Center for Cancer Research, National Cancer Institute, Bethesda, Maryland, USA Correspondence to: James H. Doroshow, email: // Keywords : NADPH oxidase, reactive oxygen species, colon cancer, interleukin-4, interleukin-13 Received : December 21, 2016 Accepted : April 17, 2017 Published : April 27, 2017 Abstract Human colon cancers express higher levels of NADPH oxidase 1 [NOX1] than adjacent normal epithelium. It has been suggested that reactive oxygen species [ROS] derived from NOX1 contribute to DNA damage and neoplastic transformation in the colon, particularly during chronic inflammatory stress. However, the mechanism(s) underlying increased NOX1 expression in malignant tumors or chronic inflammatory states involving the intestine are poorly characterized. We examined the effects of two pro-inflammatory cytokines, IL-4 and IL-13, on the regulation of NOX1. NOX1 expression was increased 4- to 5-fold in a time- and concentration-dependent manner by both cytokines in human colon cancer cell lines when a functional Type II IL-4 receptor was present. Increased NOX1 transcription following IL-4/IL-13 exposure was mediated by JAK1/STAT6 signaling, was associated with a ROS-related inhibition of protein tyrosine phosphatase activity, and was dependent upon activation and specific binding of GATA3 to the NOX1 promoter. NOX1-mediated ROS production increased cell cycle progression through S-phase leading to a significant increase in cellular proliferation. Evaluation of twenty pairs of surgically-resected colon cancers and their associated uninvolved adjacent colonic epithelium demonstrated a significant increase in the active form of NOX1, NOX1-L, in tumors compared to normal tissues, and a significant correlation between the expression levels of NOX1 and the Type II IL-4 receptor in tumor and the uninvolved colon. These studies imply that NOX1 expression, mediated by IL-4/IL-13, could contribute to an oxidant milieu capable of supporting the initiation or progression of colonic cancer, suggesting a role for NOX1 as a therapeutic target.

Published

2016

41. Abstract PD1-02: Cancer predisposition genes in metastatic breast cancer – Association with metastatic pattern, prognosis, patient and tumor characteristics

Author

Tanja Fehm, Michael Untch, Andreas Schneeweiss, Erik Belleville, D. Wallwiener, Michael P. Lux, Chunling Hu, Florin-Andrei Taran, Friedrich Overkamp, H-C Kolberg, Eric C. Polley, RD Gnanolivu, Steven N. Hart, Wolfgang Janni, Hans Tesch, Sara Y. Brucker, Jenna Lilyquist, Kun Y. Lee, D Lueftner, PA Fasching, P. Hadji, Johannes Ettl, P Wimberger, Markus Wallwiener, M. W. Beckmann, Fergus J. Couch, Andreas D. Hartkopf, Volkmar Mueller, and Lothar Haeberle

Subjects

Oncology, Cancer Research, medicine.medical_specialty, 030219 obstetrics & reproductive medicine, business.industry, BRCA mutation, Cancer, medicine.disease, Metastatic breast cancer, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Breast cancer, 030220 oncology & carcinogenesis, Internal medicine, medicine, skin and connective tissue diseases, business, Prospective cohort study, CHEK2, Brain metastasis

Abstract

Background New treatment strategies for metastatic breast cancer (mBC) are mainly driven by therapies against specific targets. BRCA mutations are one of the few established actionable targets, with PARP-Inhibitors and Platinum showing high efficacy in mBC. Hereditary cancer testing panels are now broadly used for identification of individuals with BRCA1/2 mutations who may benefit from these therapies. Many of these panels also contain other predisposition genes involved in BRCA-related DNA repair pathways, but the clinical relevance of mutations in these genes remain unclear. The aim of this study was to describe the mutation rates of BRCA1/2 and panel-based predisposition genes, and the associated clinical characteristics of individuals with these mutations, in a prospective cohort of mBC patients. Methods The PRAEGNANT mBC registry (NCT02338167) is a prospective registry for metastatic breast cancer patients with a focus on molecular biomarkers. Patients receiving any therapeutic regimen are eligible for this registry. Germline DNA was collected at study entry and genotyped for 37 cancer predisposition genes including BRCA1 and BRCA2. The frequency of mutations in each gene was determined, and associations between mutations and patient and tumor characteristics, metastatic pattern, and overall survival were assessed. Results Mutations in established high (odds ratio (OR)>5.0) and moderate risk (OR>2.0) breast cancer genes (BRCA1/2, PALB2, CHEK2, ATM, RAD51D, BARD1, and MSH6) were seen in 123 of 1462 tested patients with mBC (8.4%). BRCA1 and BRCA2 mutations were seen in 1.4% and 2.9% of patients respectively. Most frequently mutated non-BRCA panel genes were CHEK2, PALB2 and ATM with 2.8%, 0.8% and 0.6% of patients. Mutation frequency varied with regard to patients who developed brain metastases, visceral metastases or bone only metastases. BRCA1 or BRCA2 mutations were seen frequently in patients with brain (5.3%) or visceral metastases (5.2%), but were present in only 2.5% patients with bone only metastases and 1.5% of patients with lesions in other locations. Panel genes were equally distributed among all metastatic patients. PALB2 mutations (n=11) were only seen in patients with brain (1.9%) and visceral metastases (0.9%), but not in patients with bone metastases or other locations. 36.4% (N=4) of all patients with PALB2 mutations developing a brain metastasis. When adjusted for other mBC prognostic factors, a mutation (all genes) was associated with an unfavorable prognosis (HR: 1.50; 95%CI: 1.04 to 2.30, p=0.03). Mutation frequencies were similar according to therapy lines. All other associations with molecular subtypes and risk factors were similar to primary breast cancer cases. Conclusion Mutations in high and moderate risk breast cancer genes were frequent in metastatic breast cancer patients. The frequency was substantially higher than the 4 to 5% mutation frequency observed among unselected primary breast cancer patients, but is consistent with recent results from studies of metastatic prostate cancer patients. Patients with brain and visceral metastases had the highest BRCA mutation rates. Results suggested that PALB2 mutations may be more frequent in patients with brain metastases. Citation Format: Fasching PA, Hu C, Hart SN, Polley EC, Lee KY, Gnanolivu RD, Lilyquist J, Hartkopf AD, Taran FA, Janni W, Hadji P, Tesch H, Haeberle L, Ettl J, Lux MP, Lueftner D, Wallwiener M, Mueller V, Beckmann MW, Belleville E, Wimberger P, Untch M, Kolberg H-C, Fehm TN, Overkamp F, Wallwiener D, Brucker SY, Schneeweiss A, Couch F. Cancer predisposition genes in metastatic breast cancer – Association with metastatic pattern, prognosis, patient and tumor characteristics [abstract]. In: Proceedings of the 2017 San Antonio Breast Cancer Symposium; 2017 Dec 5-9; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2018;78(4 Suppl):Abstract nr PD1-02.

Published

2018

42. Abstract 4169: Population-based breast cancer risk estimates associated with cancer predisposition gene mutations from 32,298 breast cancer patients and 31,869 matched unaffected controls from the CARRIERS study

Author

Fergus J. Couch, Chunling Hu, Steven N. Hart, Rohan Gnanaolivu, Jenna Lilyquist, Kun Y. Lee, Chi Gao, Bruce Eckloff, Hoda Anton-Culver, Paul Auer, Leslie Bernstein, Mia Gaudet, Christopher Haiman, Julie Palmer, Amy Tentham-Dietz, Song Yao, Susan Domchek, Jeffrey N. Weitzel, David E. Goldgar, Katherine L. Nathanson, Peter Kraft, and Eric C. Polley

Subjects

Cancer Research, Oncology

Abstract

Clinical germline genetic testing of cancer predisposition gene panels is used to identify women at increased risk for breast cancer. Pathogenic mutations in cancer predisposition genes are associated with established risks of breast cancer and are actively used for risk management of breast cancer for women qualifying for genetic testing because of a family history of breast and/or ovarian cancer or young age of diagnosis. However, the risks of breast cancer associated with mutations in these genes have likely been overestimated for many women in the general population. The goal of the “CAnceR RIsk Estimates Related to Susceptibility” (CARRIERS) study was to estimate breast cancer risks associated with mutations in hereditary cancer panel genes. Germline DNA from 32,298 breast cancer patients and 31,869 matched unaffected controls enrolled in cohorts and population-based case-control studies were sequenced to identify pathogenic mutations in 37 cancer predisposition genes.The average age at diagnosis was 61.2 years and the average age of last follow-up was 62.1 years. DNA was subjected to dual bar-coded QIAseq multiplex PCR-based amplification of 1733 target regions in 37 predisposition genes. Products from 768 samples were pooled and sequenced in a single lane of a HiSeq 4000 system. Mutations were called by GATK Haplotype Caller and Vardict.High quality sequence data was obtained for 99.3% of target regions. Pathogenic mutations in 12 known breast cancer predisposition genes were identified in 6.2% of all breast cancer cases and 2.1% of controls; and in 6.7% of African American breast cancer cases and 1.8% of controls. In case-control association analyses adjusted for age at diagnosis or last follow up and family history of breast and ovarian cancer, mutations in BRCA1, BRCA2, and PALB2 were associated with high risks of breast cancer (odds ratio (OR)>4.0). Mutations in CHEK2 and BARD1 were associated with moderate risks of breast cancer (OR>2.0), whereas mutations in ATM had lower clinical relevance (OR=1.6). Stratification by ER, PR, and HER2 status of tumors found that BRCA1, BRCA2, PALB2 and TP53 were associated with high risks of studies of triple negative breast cancer (TNBC), and that BARD1, BRIP1, FANCM, and RAD51C were associated with moderate risks of TNBC. Overall, results from the CARRIERS study establish that mutations in predisposition genes are associated with lower risks of breast cancer in the general population than in high-risk families. The age-related estimates of breast cancer risk for each of the hereditary cancer panel genes in this study may inform on the use of cancer screening and other risk management strategies for women in the general population with mutations in predisposition genes. Citation Format: Fergus J. Couch, Chunling Hu, Steven N. Hart, Rohan Gnanaolivu, Jenna Lilyquist, Kun Y. Lee, Chi Gao, Bruce Eckloff, Hoda Anton-Culver, Paul Auer, Leslie Bernstein, Mia Gaudet, Christopher Haiman, Julie Palmer, Amy Tentham-Dietz, Song Yao, Susan Domchek, Jeffrey N. Weitzel, David E. Goldgar, Katherine L. Nathanson, Peter Kraft, Eric C. Polley. Population-based breast cancer risk estimates associated with cancer predisposition gene mutations from 32,298 breast cancer patients and 31,869 matched unaffected controls from the CARRIERS study [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 4169.

Published

2019

43. Abstract 5113: A flexible pipeline for precision medicine biomarker detection and prediction of treatment response

Author

Eric C. Polley, John K. Simmons, V Keith Hughitt, Ryan Dale, Sayeh Gorjifard, Jonathan J Keats, Beverly A. Mock, and Aleksandra M. Michalowski

Subjects

0301 basic medicine, Cancer Research, Treatment response, Computer science, Genomics, Computational biology, Precision medicine, Data type, Treatment efficacy, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, Pharmacogenomics, Profiling (information science), Exome

Abstract

Recent years have seen an explosion in the availability of paired molecular profiling and drug screen data, providing an unprecedented opportunity for the development of targeted therapies based on an individual’s genetic background. Despite a number of recent successes in diseases ranging from cystic fibrosis to cancer, significant hurdles remain in our ability to accurately predict treatments based on molecular profiling data. In particular, few such tools exist that allow the integration of heterogeneous data types (e.g. genomic, transcriptomic, and somatic mutations), along with high-throughput drug screen data to make predictions about treatment efficacy. Here, we describe a generalized open-source pipeline developed for the analysis of precision medicine data, Pharmacogenomics Prediction Pipeline, or “P3”. The modular design of P3 enables the inclusion of arbitrary input data types and the selection from multiple alternative machine learning algorithms, while automated statistical and visualization reporting steps incorporated throughout the pipeline assist in parameter tuning and early detection of problematic data components. Molecular profiling data is further enriched by the incorporation of external biological information in the form of pathway and gene set annotations such and Gene Ontology (GO) and The Molecular Signatures Database (MSigDB). To demonstrate the use of P3 for preclinical biomarker prediction, we applied P3 to an unpublished multiple myeloma dataset consisting of exome, RNA-Seq, CNV, and drug screen data for 1,912 compounds across 47 tumor cell lines. Specifically, P3 was used to predict molecular features associated with response to treatment for all drugs where a differential response to treatment was observed across patients. Furthermore, molecular profiling and drug screen data for 267 drugs and over a thousand cell lines spanning multiple cancer types from the Genomics of Drug Sensitivity in Cancer (GDSC) project were analyzed using P3, providing insights into shared mechanisms of drug sensitivity and resistance across different cancer and treatment types. Citation Format: V Keith Hughitt, Sayeh Gorjifard, Aleksandra M. Michalowski, John K. Simmons, Ryan Dale, Eric C. Polley, Jonathan J. Keats, Beverly A. Mock. A flexible pipeline for precision medicine biomarker detection and prediction of treatment response [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 5113.

Published

2019

44. Abstract 4177: The joint effects of polygenic risk scores and pathogenic variants in cancer predisposition genes on breast cancer risk in the general population: results from the CARRIERS study

Author

Hoda Anton-Culver, Nicholas J. Boddicker, Jeffrey N. Weitzel, Josh Klebba, Paul L. Auer, Peter Kraft, Leslie R. Bernstein, Chi Gao, Chunling Hu, Christopher A. Haiman, Amy Trentham-Dietz, Katherine L. Nathanson, Bruce W. Eckloff, Fergus J. Couch, Jenna Lilyquist, Rohan Gnanaolivu, Susan M. Domchek, Eric C. Polley, Mia M. Gaudet, David E. Goldgar, Janet E. Olson, Song Yao, Raed Samara, Julie R. Palmer, Kun Y. Lee, and Steven N. Hart

Subjects

Oncology, Cancer Research, medicine.medical_specialty, education.field_of_study, business.industry, PALB2, Population, Haplotype, Cancer, Genome-wide association study, medicine.disease, MLH1, Breast cancer, CDKN2A, Internal medicine, medicine, education, business

Abstract

Background: Understanding the joint effect on breast cancer risk of rare pathogenic variants in cancer predisposition genes and polygenic risk scores (PRS) from common variants can enable a precision approach to breast cancer management. Previous work found that PRS were associated with breast cancer risk in BRCA1 and BRCA2 mutation carriers recruited from cancer genetics clinics (Kuchenbaecker et al. JNCI 2017). The joint effects of pathogenic variants and PRS have not been studied in samples drawn from the general population. There is also no existing study evaluating the effect of PRS in mutation carriers in genes other than BRCA1/2. Here we evaluate the joint effects of PRS and pathogenic mutations in established cancer predisposition genes in a population-based case-control sample. Method: We analyzed 53,199 European-ancestry individuals (20,730 controls and 21,272 cases) drawn from 7 cohorts and 2 population-based case-control studies in the CAnceR RIsk Estimates Related to Susceptibility” (CARRIERS) consortium. Targeted sequencing was performed using dual bar-coded QIAseq. Mutation calling was conducted with Haplotype Caller and Vardict. We sequenced 18 breast cancer predisposition genes: ATM, BARD1, BRCA1, BRCA2, BRIP1, CDH1, CDKN2A, CHECK2, FANCC, MLH1, MSH2, MSH6, NF1, PALB2, PTEN, RAD51C, RAD51D and TP53. The PRS was calculated based on 128 common variants using effect estimates from the largest published breast cancer GWAS. The PRS was standardized to a mean of 0 and standard deviation of 1. Logistic regression was performed to assess the combined effect of identified mutation and common variants (including main and interaction effects for carrier status and PRS). Results: A total of 1,770 pathogenic mutations were observed. About 1% of the study sample had mutations in either BRCA1 (n=209) or BRCA2 gene (n=305), and 2.2% had mutations in other genes (n=1,176). The effect of PRS in BRCA1 carriers was OR= 0.97 (95%CI: 0.62, 1.52); however, this is not statistically significantly different from the PRS in non-carriers [OR=1.23 (95%CI: 1.20, 1.25)] or previous estimates in carriers [OR: 1.14, 95%CI: 1.11-1.17]. The effect of PRS in BRCA2 carriers was OR=1.87 (95%CI: 1.31, 2.78) which was statistically significantly different from that of the non-carriers. Among the mutation carriers in genes other than BRCA, the effect of PRS on breast cancer was OR=1.00 (95%CI: 0.88,1.15). Conclusion: Consistent with previous studies, we did not find evidence that the effect of the PRS among BRCA1 carriers was statistically significantly different than non-carriers. We found some evidence that the PRS effect may be larger among BRCA2 carriers than non-carriers. Our results also suggest that PRS may not have a strong effect on breast cancer risk in mutation carriers of other predisposition genes; further work is needed for verification. Citation Format: Chi Gao, Chunling Hu, Steven N. Hart, Rohan Gnanaolivu, Kun Y. Lee, Jenna Lilyquist, Nicholas J. Boddicker, Bruce Eckloff, Raed Samara, Josh Klebba, Paul Auer, Leslie Bernstein, Mia Gaudet, Hoda Anton-Culver, Amy Trentham-Dietz, Julie R. Palmer, Song Yao, Christopher Haiman, Janet E. Olson, Susan Domchek, Jeffrey Weitzel, David Goldgar, Katherine L. Nathanson, Eric C. Polley, Fergus J. Couch, Peter Kraft. The joint effects of polygenic risk scores and pathogenic variants in cancer predisposition genes on breast cancer risk in the general population: results from the CARRIERS study [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 4177.

Published

2019

45. Genetic predisposition to breast cancer among African American women

Author

Mia M. Gaudet, David E. Goldgar, Leslie Bernstein, Amy Trentham-Dietz, Steven N. Hart, Chunling Hu, Jeffrey N. Weitzel, Susan M. Domchek, Fergus J. Couch, Peter Kraft, Julie R. Palmer, Hoda Anton-Culver, Eric C. Polley, Christopher A. Haiman, Esther M. John, Song Yao, Katherine L. Nathanson, Rohan Gnanaolivu, Tuya Pal, and Chi Gao

Subjects

African american, Oncology, Cancer Research, medicine.medical_specialty, business.industry, medicine.disease, Breast cancer susceptibility genes, Breast cancer, Internal medicine, medicine, Genetic predisposition, Clinical genetic, Identification (biology), skin and connective tissue diseases, business

Abstract

104 Background: The identification of pathogenic mutations in breast cancer susceptibility genes through clinical genetic testing leads to focused screening and prevention strategies for women at increased risk of cancer. However, the frequency of mutations and the risks of cancer associated with breast cancer predisposition genes has not been established for the African American population. Methods: Germline DNA samples from African American women (5,054 breast cancer cases and 4,993 age-matched unaffected controls) from 10 U.S. studies were tested for mutations in 20 established breast cancer predisposition genes using a QIAseq multiplex amplicon panel as part of the “CAnceR RIsk Estimates Related to Susceptibility” (CARRIERS) study. The frequency of mutations in each gene and associations between mutations and breast cancer risk, adjusted for study design, age, and first-degree family history of breast cancer, were evaluated. Results: The mean age at diagnosis of breast cancer cases was 54.4 years and the mean age of controls was 55.2 years. 18.2% of cases and 10.8% of controls reported a first-degree family history of breast cancer. Pathogenic mutations in any of the 20 breast cancer predisposition genes were identified in 7.6% of breast cancer cases and 2.4% of controls. In multivariable analyses, mutations in BRCA1, BRCA2, and PALB2 were associated with high risks of breast cancer (odds ratio (OR) > 5.0). Mutations in CHEK2 were associated with moderate risks of breast cancer (OR > 2.0), whereas mutations in ATM had lower clinical relevance (OR = 1.8). Mutations in BRCA1, BRCA2, PALB2, and RAD51D, but not CHEK2 or ATM, were associated with increased risks of estrogen receptor negative breast cancer. Conclusions: Cancer predisposition genes confer similar risks of breast cancer in the African American population as in non-Hispanic Whites. These studies provide important insights into the risks of breast cancer associated with predisposition gene mutations in the African American population.

Published

2019

46. Racial and ethnic differences in the results of multigene panel testing of inherited cancer predisposition genes in breast cancer patients

Author

David E. Goldgar, Chunling Hu, Hermela Shimelis, Steven N. Hart, Holly LaDuca, Amal Yussuf, Stephanie Gutierrez, Jill S. Dolinsky, Elizabeth C. Chao, Siddhartha Yadav, Jenna Lilyquist, Eric C. Polley, Tina Pesaran, Fergus J. Couch, Brigette Tippin Davis, Jie Na, Kun Lee, and Nancy Niguidula

Subjects

Oncology, Cancer Research, medicine.medical_specialty, business.industry, Cancer predisposition, Ethnic group, medicine.disease, Germline, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Germline mutation, 030220 oncology & carcinogenesis, Internal medicine, medicine, skin and connective tissue diseases, business, Gene, 030215 immunology

Abstract

1514 Background: The prevalence of germline mutations in non-white patients with breast cancer and the germline genetic drivers of breast cancer risk in non-white populations are largely unknown. Methods: The study population included 77,900 women with breast cancer (Non-Hispanic white: 57,003; Black: 6,722; Asian: 4,183; Hispanic: 5,194; Ashkenazi-Jewish: 4,798) who underwent germline multigene panel testing of cancer predisposition genes from March 2012 to December 2016. The prevalence of predisposition gene mutations in racial and ethnic populations relative to non-Hispanic Whites was assessed while accounting for age at diagnosis of breast cancer, family history of breast and ovarian cancer, and estrogen receptor status of breast tumors. Associations between mutations in each gene and breast cancer risk were evaluated using reference controls. Results: The overall frequency of pathogenic mutations in known breast cancer predisposition genes was 9.1% for non-Hispanic Whites, 9.8% for African Americans, 10.2% for Hispanics, 7.6% for Ashkenazi-Jewish, and 7.5% for Asians. BRCA1 mutations were enriched (p < 0.05) and CHEK2 mutations were under-represented in all racial and ethnic populations relative to non-Hispanic Whites. BRCA2 and BARD1 mutations were enriched in African Americans and Hispanics relative to non-Hispanic Whites, whereas PALB2 and RAD51C mutations were enriched in Hispanics. Among genes with mutation counts large enough for assessment, mutations in BARD1, BRCA1, BRCA2, PALB2 and TP53 were significantly associated with clinically relevant increased risks (odds ratio (OR) > 2) of breast cancer across all ethnicities and races. Rates of variants of uncertain significance were highest among Asians (29%), followed by blacks (27%), Hispanics (21%), non-Hispanic whites (16%) and Ashkenazi-Jews (14%). Conclusions: While there is some similarity across ethnic groups, substantial heterogeneity exists in the prevalence of mutations in breast cancer predisposition genes across major racial and ethnic groups in the US population. These findings contribute to our understanding of breast cancer risk and have significant implications for genetic testing, screening, and management of patients with an inherited predisposition to breast cancer, with a need for continued analysis with increased cohort size in ethnic minority groups.

Published

2019

47. Abstract GS2-01: Age-related breast cancer risk estimates for the general population based on sequencing of cancer predisposition genes in 19,228 breast cancer patients and 20,211 matched unaffected controls from US based cohorts in the CARRIERS study

Author

Bruce W. Eckloff, Josh Klebba, Chunling Hu, Christopher A. Haiman, Fergus J. Couch, Rohan Gnanaolivu, Leslie R. Bernstein, Chi Gao, Susan M. Domchek, David E. Goldgar, Julie R. Palmer, Song Yao, Katherine L. Nathanson, Raed Samara, Eric C. Polley, Paul W. Auer, Jenna Lilyquist, Steven N. Hart, Jeffrey N. Weitzel, Mia M. Gaudet, Peter Kraft, and Kun Y. Lee

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Population, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Internal medicine, medicine, skin and connective tissue diseases, education, CHEK2, Triple-negative breast cancer, Genetic testing, education.field_of_study, medicine.diagnostic_test, business.industry, Cancer, Odds ratio, medicine.disease, 030104 developmental biology, 030220 oncology & carcinogenesis, business, Ovarian cancer

Abstract

Background: Clinical germline genetic testing of cancer predisposition gene panels is used to identify women at increased risk for breast cancer. The identification of pathogenic mutations in established high and moderate predisposition genes may result in improved risk management of breast cancer for tested patients and their family members through tailored screening, prophylactic surgeries, or chemoprevention. However, the risks of breast cancer associated with mutations in these genes have likely been overestimated for many women in the general population because previous studies have focused on individuals with a family history of breast and/or ovarian cancer, early onset disease, or triple negative breast cancer. The goal of the “CAnceR RIsk Estimates Related to Susceptibility” (CARRIERS) study is to estimate breast cancer risks associated with mutations in hereditary cancer panel genes in the general population. Methods: Germline DNA samples from blood or saliva were obtained from 39,439 breast cancer patients and matched unaffected controls from six US-based cohorts (BWHS, CPSII, CTS, MEC, NHS1, NHS2, WHI). DNA was subjected to dual bar-coded QIAseq multiplex PCR-based amplification of 1733 target regions covering all coding regions of 37 cancer predisposition genes and sequenced. Mutation calling was conducted with Haplotype Caller and Vardict. Results: High quality sequence data was obtained for 38,990 of 39,439 samples (98.9%) and for 99.3% of target regions. Pathogenic mutations in 12 known breast cancer predisposition genes were identified 4.5% of all breast cancer cases and 2.1% of controls; and in 6.7% of African American breast cancer cases and 1.8% of controls. Differences in mutation frequencies were observed by age with mutations in 7.8% of cases diagnosed £50 years of age and 4.0% of cases diagnosed over age 50. Mutations in ATM, BRCA1, BRCA2, and PALB2 were enriched 2 to 3-fold in cases diagnosed under age 50 relative to older cases. No change in frequency of CHEK2 mutations by age was observed. In case-control analyses mutations in BRCA1, BRCA2 and PALB2 were significantly associated with a high risk of breast cancer (odds ratio (OR)>4.0). Of these, BRCA1 and BRCA2 displayed ORs of 13.5 and 16.6 in the £50 age group, but only 5.7 and 3.2 in the >50 age group. Only minor age-specific effects were observed for PALB2. Mutations in ATM and CHEK2 were associated with moderate risks of breast cancer (OR=2.0 to 4.0) in the younger age group, but not in the older age group. Conclusions: Results from the CARRIERS cohort-based study establish that mutations in known breast cancer predisposition genes are associated with only moderate risks of breast cancer in the general population. However, risks are substantially increased for BRCA1 and BRCA2 but not ATM, CHEK2 or PALB2 mutations in those £50 years of age. The age-related estimates of breast cancer risk for each of the hereditary cancer panel genes in this study may inform selection of individuals in the general population who may benefit from genetic testing and associated risk management strategies. Citation Format: Couch FJ, Hu C, Hart SN, Gnanaolivu RD, Lilyquist J, Lee KY, Gao C, Eckloff B, Samara R, Klebba J, Auer P, Bernstein L, Gaudet M, Haiman C, Palmer JR, Yao S, Domchek SM, Weitzel JN, Goldgar DE, Nathanson KL, Kraft P, Polley EC. Age-related breast cancer risk estimates for the general population based on sequencing of cancer predisposition genes in 19,228 breast cancer patients and 20,211 matched unaffected controls from US based cohorts in the CARRIERS study [abstract]. In: Proceedings of the 2018 San Antonio Breast Cancer Symposium; 2018 Dec 4-8; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2019;79(4 Suppl):Abstract nr GS2-01.

Published

2019

48. The Exomes of the NCI-60 Panel: A Genomic Resource for Cancer Biology and Systems Pharmacology

Author

Ogan D. Abaan, Eric C. Polley, Yevgeniy Gindin, Paul S. Meltzer, Sven Bilke, William C. Reinhold, Susan Holbeck, Yuelin J. Zhu, Richard M. Simon, Yuan Jiang, Robert L. Walker, James H. Doroshow, Yves Pommier, Marbin Pineda, and Sean Davis

Subjects

Cancer Research, media_common.quotation_subject, Antineoplastic Agents, Biology, Article, Ingenuity, Cell Line, Tumor, Neoplasms, medicine, Humans, Exome, Vemurafenib, Exome sequencing, media_common, Genetics, Genetic Variation, Cancer, medicine.disease, Oncology, Pharmacogenetics, Pharmacogenomics, Mutation, Erlotinib, Drug Screening Assays, Antitumor, Systems pharmacology, medicine.drug

Abstract

The NCI-60 cell lines are the most frequently studied human tumor cell lines in cancer research. This panel has generated the most extensive cancer pharmacology database worldwide. In addition, these cell lines have been intensely investigated, providing a unique platform for hypothesis-driven research focused on enhancing our understanding of tumor biology. Here, we report a comprehensive analysis of coding variants in the NCI-60 panel of cell lines identified by whole exome sequencing, providing a list of possible cancer specific variants for the community. Furthermore, we identify pharmacogenomic correlations between specific variants in genes such as TP53, BRAF, ERBBs, and ATAD5 and anticancer agents such as nutlin, vemurafenib, erlotinib, and bleomycin showing one of many ways the data could be used to validate and generate novel hypotheses for further investigation. As new cancer genes are identified through large-scale sequencing studies, the data presented here for the NCI-60 will be an invaluable resource for identifying cell lines with mutations in such genes for hypothesis-driven research. To enhance the utility of the data for the greater research community, the genomic variants are freely available in different formats and from multiple sources including the CellMiner and Ingenuity websites. Cancer Res; 73(14); 4372–82. ©2013 AACR.

Published

2013

49. RefCNV: Identification of Gene-Based Copy Number Variants Using Whole Exome Sequencing

Author

Lun-Ching Chang, Han Si, Chih Jian Lih, Paul M. McGregor, Corinne Camalier, Biswajit Das, and Eric C. Polley

Subjects

0301 basic medicine, Cancer Research, business.industry, Methodology, copy number variation, Genomics, Computational biology, Bioinformatics, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, DNA sequencing, whole exome sequencing, Correlation, 03 medical and health sciences, Exon, 030104 developmental biology, Oncology, Medicine, next-generation sequencing, Digital polymerase chain reaction, Copy-number variation, business, Gene, Exome sequencing

Abstract

With rapid advances in DNA sequencing technologies, whole exome sequencing (WES) has become a popular approach for detecting somatic mutations in oncology studies. The initial intent of WES was to characterize single nucleotide variants, but it was observed that the number of sequencing reads that mapped to a genomic region correlated with the DNA copy number variants (CNVs). We propose a method RefCNV that uses a reference set to estimate the distribution of the coverage for each exon. The construction of the reference set includes an evaluation of the sources of variability in the coverage distribution. We observed that the processing steps had an impact on the coverage distribution. For each exon, we compared the observed coverage with the expected normal coverage. Thresholds for determining CNVs were selected to control the false-positive error rate. RefCNV prediction correlated significantly ( r = 0.96–0.86) with CNV measured by digital polymerase chain reaction for MET (7q31), EGFR (7p12), or ERBB2 (17q12) in 13 tumor cell lines. The genome-wide CNV analysis showed a good overall correlation (Spearman's coefficient = 0.82) between RefCNV estimation and publicly available CNV data in Cancer Cell Line Encyclopedia. RefCNV also showed better performance than three other CNV estimation methods in genome-wide CNV analysis.

Published

2016

50. Expanding BRCA1/2 testing criteria to include other confirmed breast and ovarian cancer susceptibility genes

Author

Jill S. Dolinsky, Jenna Lilyquist, Chunling Hu, Carolyn Horton, Hermela Shimelis, Fergus J. Couch, Holly LaDuca, Eric C. Polley, Steven N. Hart, Virginia Speare, Amal Yussuf, and Lily Hoang

Subjects

Oncology, Cancer Research, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Cancer, Susceptibility gene, medicine.disease, Internal medicine, medicine, Ovarian cancer, business, Genetic testing

Abstract

1524Background: The National Comprehensive Cancer Network (NCCN) has expanded its breast and ovarian cancer (BC and OC) genetic testing and management recommendations to address the broader spectru...

Published

2018