The association between germline <scp><i>BRCA2</i></scp> variants and sensitivity to platinum‐based chemotherapy among men with metastatic prostate cancer

Pomerantz, Mark; Spisák, Sándor; Li, Jia; Cronin, Angel M.; Csabai, István; Ledet, Elisa M.; Sartor, A. Oliver; Rainville, Irene; O’Connor, Edward; Herbert, Zachary T.; Szállási, Zoltán; Oh, William K.; Kantoff, Philip W.; Garber, Judy E.; Schrag, Deborah; Kibel, Adam S.; Freedman, Matthew L.

doi:10.1002/cncr.30808

Cited by 225 publications

(186 citation statements)

References 39 publications

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“…Mutations are associated with lifetime risks of 80% for breast cancer and 15%-40% for cancer of the ovary or fallopian tube for BRCA2 and BRCA1 respectively 3 . BRCA2 is the most frequently mutated gene in both prostate cancer 4,5 and pancreatic cancer [6][7][8] , and patients with BRCA2 mutations can benefit from novel therapies such as cis-platinum 9 . Annually, about 8500 cases of prostate cancer and 2150 cases of pancreatic cancer are diagnosed in Ontario, but very few of those patients are being tested for BRCA2.…”

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confidence: 99%

Coming of Age in Canada: A Study of Population-Based Genetic Testing for Breast and Ovarian Cancer

2017

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The BRCA1 and BRCA2 genes are the two most commonly mutated in hereditary breast and ovarian cancer, and they are the canonical pair when it comes to cancer testing 1 . There are many other candidate genes, and large-panel testing is increasingly the norm even though not all practitioners are in agreement 2 that testing for 20 genes is better than testing for 2. Mutations are associated with lifetime risks of 80% for breast cancer and 15%-40% for cancer of the ovary or fallopian tube for BRCA2 and BRCA1 respectively 3 . BRCA2 is the most frequently mutated gene in both prostate cancer 4,5 and pancreatic cancer [6][7][8] , and patients with BRCA2 mutations can benefit from novel therapies such as cis-platinum 9 . Annually, about 8500 cases of prostate cancer and 2150 cases of pancreatic cancer are diagnosed in Ontario, but very few of those patients are being tested for BRCA2.Genetic screening is now mainstream as a consequence of diminished sequencing costs, increased public awareness, celebrity endorsement, and the now wide availability to women of preventive surgery through public and private health insurance. Intensified screening for mutation carriers with annual magnetic resonance imaging is advocated and is increasingly available 10 . Additionally, women with hereditary breast cancer can benefit from personalized treatment (both surgical and medical), which might include bilateral mastectomy, salpingo-oophorectomy, and tailored chemotherapy (cis-platinum or olaparib) 11 .The current model of delivering genetic testing for the BRCA genes in North America dates to the mid-1990s, at a time when genetic testing was expensive and the clinical benefits were largely unproven. Because of the high cost, public and private insurers were not willing to pay for testing for all comers. In the resulting model, a women is referred by her physician to a specialized cancer genetics clinic, where a formal assessment is conducted. If the risk estimate for carrying a mutation exceeds a threshold value (usually 10%), then genetic testing for the BRCA genes ensues. If not, then the woman is reassured and sent off with a number of recommendations based on her personal and family history of cancer. In many clinics, the volume of patient requests now exceeds the number of available appointments, and triage is conducted by mail or telephone. The genetics counsellor serves two purposes: informing women about cancer risk, management options, and the testing process; and ensuring that testing is rationed first to the women who are the most suitable candidates.We believe that the current model is outdated, and here we propose an alternative model based on direct-toconsumer population-based testing. The reasons are these:■ First, a significant proportion of BRCA mutation carriers do not reach the 10% threshold; they therefore represent missed opportunities for identification 12 . ■ Very few patients with prostate cancer or pancreatic cancer are being tested. In addition, many individuals who do qualify for genetic testing fail to be ide...

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confidence: 99%

Coming of Age in Canada: A Study of Population-Based Genetic Testing for Breast and Ovarian Cancer

2017

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“…Personalized therapy of advanced metastatic prostate cancer has entered a new phase since the demonstration of the clinical efficacy of PARP inhibitors and platinum in cases with germline mutations in the DNA repair pathway, especially homologous recombination [4,24]. However, some of the DNA damage checkpoint gene germline mutants do not benefit from PARP inhibitor therapy [25] and some cases without such germline mutations are sensitive to platinum-based therapy [24,26]. Therefore, optimal use of these therapeutic approaches will require more accurate identification of HR deficient cases.…”

Section: Discussionmentioning

confidence: 99%

Genomic aberration based molecular signatures efficiently characterize homologous recombination deficiency in prostate cancer

Sztupinszki

Dióssy

Krzystanek

et al. 2019

Preprint

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Background: Prostate cancers with mutations in genes involved in homologous recombination (HR), most commonly BRCA2, respond favorably to PARP inhibition and platinum-based chemotherapy. It is not clear, however, whether other prostate tumors that do not harbor deleterious mutations in these particular genes can similarly be deficient in HR, rendering them sensitive to HR-directed therapies.To identify a more comprehensive set of prostate cancer cases with homologous recombination deficiency (HRD) including those cases that do not harbor mutations in known HR genes.HRD levels can be estimated using various mutational signatures derived from nextgeneration sequencing data. We used this approach to determine whether prostate cancer cases display clear signs of HRD in somatic tumor biopsies. Whole genome (n=311) and whole exome sequencing data (n=498) of both primary and metastatic prostate adenocarcinomas (PRAD) were analyzed.Results: Known BRCA-deficient samples showed robust signs of HR-deficiency associated mutational signatures. HRD-patterns were also detected in a subset of patients who did not harbor germline or somatic mutations in BRCA1/2 or other HR related genes. Patients with HRD signatures had a significantly worse prognosis than patients without signs of HRD. Conclusions:These findings may expand the number of cases likely to respond to PARPinhibitor treatment. Based on the HRD associated mutational signatures, 5-8 % of prostate cancer cases may be good candidates for PARP-inhibitor treatment (including those with BRCA1/2 mutations).3 Key words: BRCA1, BRCA2, DNA repair genes, homologous recombination deficiency, PARP inhibitors, Prostate cancer somatic mutations in BRCA1/2 or other HR related genes. This likely defines a subset of prostate cancer patients that will likely benefit from PARP inhibitor or platinum-based therapy.

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“…To date, there have been scattered case reports of men with mCRPC harboring BRCA2 mutations who had dramatic responses to platinum chemotherapy . In this issue of Cancer , Pomerantz and colleagues describe the largest cohort of men to date with identified BRCA2 mutations who received treatment with carboplatin. On a prospective, institutional review board‐approved protocol at Dana Farber Cancer Institute, this team identified 141 men with mCRPC who had blood samples available for DNA extraction (almost all of whom had failed prior docetaxel monotherapy) and received had treatment with combined carboplatin and docetaxel.…”

Section: Selected Ongoing Clinical Trials Using Parp Inhibitors In Prmentioning

confidence: 99%

Exploiting DNA damage without repair: The activity of platinum chemotherapy in BRCA‐mutated prostate cancers

Humeniuk

Zhang

Armstrong

2017

Cancer

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The association between germline BRCA2 variants and sensitivity to platinum‐based chemotherapy among men with metastatic prostate cancer

Cited by 225 publications

References 39 publications

Coming of Age in Canada: A Study of Population-Based Genetic Testing for Breast and Ovarian Cancer

Coming of Age in Canada: A Study of Population-Based Genetic Testing for Breast and Ovarian Cancer

Genomic aberration based molecular signatures efficiently characterize homologous recombination deficiency in prostate cancer

Exploiting DNA damage without repair: The activity of platinum chemotherapy in BRCA‐mutated prostate cancers

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