Detection of BRCA1, BRCA2, and ATM Alterations in Matched Tumor Tissue and Circulating Tumor DNA in Patients with Prostate Cancer Screened in PROfound

N., Kim; Barnicle, Alan; Sibilla, Caroline; Lai, Zhongwu; Corcoran, Claire; Barrett, J. Carl; Adelman, Carrie A.; Qiu, Ping; Easter, Ashley; Dearden, Simon; Oxnard, Geoffrey R.; Agarwal, Neeraj; Azad, Arun; Bono, Johann S. de; Mateo, Joaquín; Olmos, David; Thiery-Vuillemin, A.

doi:10.1158/1078-0432.ccr-22-0931

Cited by 32 publications

(22 citation statements)

References 47 publications

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“…These data are consistent with the prior studies [ 14 , 18 , 19 ]. Tukachinsky and colleagues reported that with tumor tissue as reference, the positive percentage agreement for BRCA1/2 on cfDNA was 93% [ 14 ].…”

Section: Discussionsupporting

confidence: 94%

Detection of BRCA1, and BRCA2 Alterations in Matched Tumor Tissue and Circulating Cell-Free DNA in Patients with Prostate Cancer in a Real-World Setting

McFarland

Thomas

Nussenzveig³

et al. 2022

Biomedicines

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Background: Poly (ADP-ribose) polymerase (PARP) inhibitors are approved for patients with metastatic castration-resistant prostate cancer harboring deleterious or suspected deleterious BRCA1 and/or 2 mutations. Identifying patients with prostate cancer harboring these mutations may be challenging. Circulating cell-free DNA (cfDNA) provides an avenue for an easier detection of these mutations. Herein, we aimed to evaluate the concordance of BRCA mutations in the tumor tissue and cfDNA in patients with metastatic prostate cancer in the real-world setting. Methods: Somatic genomic profiling results were obtained from a clinical cohort of patients at our institution who had at least two samples tested. One of the samples needed to be from either primary or metastatic tissue. Concordance was adjusted to not include mutation types that the cfDNA platforms were not designed to detect. Results: The presence or absence of mutations in the BRCA gene was assessed in a total of 589 samples, including 327 cfDNA samples, from 260 patients with metastatic prostate cancer. The median time between the first test and any subsequent test was 22.8 (0.0–232) months. BRCA mutation was present in the patient’s original prostate tissue in 23 samples (3.9%) of patients. The adjusted concordance between prostate tumor tissue and cfDNA was 97.9% [95% CI, 95.3–99.1%]. The adjusted concordance between metastatic samples and cfDNA was 93.5% [95% CI, 86.4–97.3%]. Of the patients who had a BRCA mutation detected in their prostate tissue, there was a 70% probability of detecting a BRCA mutation in the patient’s cfDNA as well. For patients who did not have a detectable BRCA mutation in their primary prostate tissue, the probability of detecting a subsequent one later in the disease course was less than 0.9%. Conclusion: There is a high level of concordance between tissue and blood for BRCA mutations. Testing cfDNA can provide reliable information on BRCA mutational status and is a viable alternative to solid tissue sequencing when unavailable. The development of a new BRCA mutation later in the disease course is a rare event.

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Section: Discussionsupporting

confidence: 94%

Detection of BRCA1, and BRCA2 Alterations in Matched Tumor Tissue and Circulating Cell-Free DNA in Patients with Prostate Cancer in a Real-World Setting

McFarland

Thomas

Nussenzveig³

et al. 2022

Biomedicines

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“…15-20% of mCRPC harbor deleterious HRR-related gene mutations, most commonly in BRCA2, ATM and CDK12. Concordance between tissue and ctDNA for HRR gene mutations is excellent, exceeding 90% in most studies (23,64,71,78,79). However, an HRR-related gene mutation alone may be insufficient to confer therapeutic vulnerability.…”

Section: Homologous Recombination Repair Deficiencymentioning

confidence: 97%

“…These resourcing requirements mean that a majority of clinicians around the world continue to have limited access to ctDNA profiling to inform patient care. Instead, clinicians typically encounter ctDNA testing in the clinical trial setting, where it is increasingly used alongside tumor tissue testing to screen for genomic alterations that may confer sensitivity to established and novel targeted therapies (20)(21)(22)(23)(24)(25). Outside of clinical trials, US FDAapproved commercial platforms are available (e.g., FoundationOne Liquid CDx, Guardant360 CDx) (26, 27), but can be cost prohibitive for patients unable to acquire partial or full financial reimbursement for testing.…”

Section: Clinical Applicationsmentioning

confidence: 99%

“…However, plasma ctDNA screening is increasingly used to complement or replace existing screening procedures. Recent PARP inhibitor studies in mCRPC have endorsed ctDNA analysis alongside tumor tissue testing to cross-validate presence of HRR alterations (20)(21)(22)(23). PC-BETS (IND.234) and ProBio are two ongoing biomarker-directed prospective mCRPC clinical trials utilizing cfDNA testing for treatment allocation (25,93).…”

Section: Ctdna For Clinical Trial Eligibilitymentioning

confidence: 99%

“…Many commercial and academic plasma cfDNA assays are capable of detecting somatic mutations below 1% ctDNA, but heterozygous and homozygous deletions typically require far greater ctDNA to be reliably detected ( 78 , 82 , 83 ). Therefore, low ctDNA% may be a limiting factor in detecting HRR alterations in cfDNA, especially large structural rearrangements and homozygous deletion events ( 23 ).…”

Section: Clinical Applicationsmentioning

confidence: 99%

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Towards clinical implementation of circulating tumor DNA in metastatic prostate cancer: Opportunities for integration and pitfalls to interpretation

Kwan

Wyatt

2022

Front. Oncol.

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Plasma circulating tumor DNA (ctDNA) represents short fragments of tumor-derived DNA released into the bloodstream primarily from cancer cells undergoing apoptosis. In metastatic castration-resistant prostate cancer (mCRPC), characterizing genomic alterations in ctDNA identifies mutations, copy number alterations, and structural rearrangements with predictive and prognostic biomarker utility. These associations with clinical outcomes have resulted in ctDNA increasingly incorporated into routine clinical care. In this review, we summarize current and emerging applications for ctDNA analysis in metastatic prostate cancer, including outcome prediction, treatment selection, and characterization of treatment resistance. We also discuss potential pitfalls with interpreting ctDNA findings, namely false negatives arising from low tumor content and optimal assay design, including correction for clonal hematopoiesis of indeterminate potential and germline variants. Understanding the influence of these limitations on interpretation of ctDNA results is necessary to overcome barriers to clinical implementation. Nevertheless, as assay availability and technology continue to improve, recognizing both opportunities and shortcomings of ctDNA analysis will retain relevance with informing the implementation of precision-oncology initiatives for metastatic prostate cancer.

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Preservation of cfRNA in cytological supernatants for cfDNA & cfRNA double detection in non‐small cell lung cancer patients

Ma,

Wang,

et al. 2024

Cancer Medicine

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BackgroudSupernatants from various cytological samples, including body cavity effusion, sputum, bronchoalveolar lavage fluid (BALF), and needle aspiration, have been validated for detecting genetic alterations using cell‐free DNA (cfDNA) in patients with non‐small cell lung cancer (NSCLC). However, the sensitivity of fusion variations detection remains challenging. The protection of cell‐free RNA (cfRNA) is critical for resolving the issue.MethodsA protective solution (PS) was applied for preserving cfRNA in cytological supernatant (CS), and the quality of protected cfRNA was assessed by cycle threshold (CT) values from reverse transcription quantitative polymerase chain reaction (RT‐qPCR). Furthermore, we collected an additional set of malignant cytological and matched tumor samples from 84 NSCLC patients, cfDNA & cfRNA extraction and double detection for driver gene mutations was validated using the multi‐gene mutations detection by RT‐qPCR.ResultsUnder the optimal protection system, 91.0% (101/111) of cfRNA were protected effectively. Among the 84 NSCLC patient samples, seven cytological samples failed the tests. In comparison with tumor samples, the overall sensitivity and specificity of detecting driver genes of supernatant cfDNA and cfRNA were 93.8% (74/77) and 100% (77/77), respectively. Notably, when focusing exclusively on patients with fusion gene changes, both sensitivity and specificity reached 100% (11/11) for EML4‐ALK, ROS1, RET fusions, and MET ex14 skipping.ConclusionThese findings suggest that cfDNA & cfRNA extraction and double detection strategy recommended in this study improve the accuracy of driver genes mutations test, especially for RNA‐based assay.

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Detection of BRCA1, BRCA2, and ATM Alterations in Matched Tumor Tissue and Circulating Tumor DNA in Patients with Prostate Cancer Screened in PROfound

Cited by 32 publications

References 47 publications

Detection of BRCA1, and BRCA2 Alterations in Matched Tumor Tissue and Circulating Cell-Free DNA in Patients with Prostate Cancer in a Real-World Setting

Detection of BRCA1, and BRCA2 Alterations in Matched Tumor Tissue and Circulating Cell-Free DNA in Patients with Prostate Cancer in a Real-World Setting

Towards clinical implementation of circulating tumor DNA in metastatic prostate cancer: Opportunities for integration and pitfalls to interpretation

Preservation of cfRNA in cytological supernatants for cfDNA & cfRNA double detection in non‐small cell lung cancer patients

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