The Impact of Foundation Medicine Testing on Cancer Patients: A Single Academic Centre Experience

Karol, Dalia; Mckinnon, M.; Mukhtar, Lenah; Awan, Arif; Lo, Bryan; Wheatley‐Price, Paul

doi:10.3389/fonc.2021.687730

Cited by 12 publications

(15 citation statements)

References 22 publications

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“…The most commonly altered genes by genetic variation of class 4-5 and VUS in this study were consistent with those published in the literature, with TP53 as the most common gene, followed by RAS, PIK3CA, and CDKN2A/B (15,16,19,20). In the present Cancers for which more than five patients had available sequencing results were analyzed.…”

Section: Discussionsupporting

confidence: 90%

“…The success rate was 78% for liquid biopsy samples and 88% for FFPE samples (40% of biopsies), indicating that the ability to detect alterations is lower for liquid biopsies. These data are consistent with the literature comparing liquid and tissue biopsy samples (14)(15)(16)(17)(18). Takeda et al showed that the success rate of the NGS assay performed with FFPE samples, including 34% of biopsy specimens, was 96.7% in different types of cancer (19).…”

Section: Discussionsupporting

confidence: 90%

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Clinical management of molecular alterations identified by high throughput sequencing in patients with advanced solid tumors in treatment failure: Real-world data from a French hospital

et al. 2023

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BackgroundIn the context of personalized medicine, screening patients to identify targetable molecular alterations is essential for therapeutic decisions such as inclusion in clinical trials, early access to therapies, or compassionate treatment. The objective of this study was to determine the real-world impact of routine incorporation of FoundationOne analysis in cancers with a poor prognosis and limited treatment options, or in those progressing after at least one course of standard therapy.MethodsA FoundationOneCDx panel for solid tumor or liquid biopsy samples was offered to 204 eligible patients.ResultsSamples from 150 patients were processed for genomic testing, with a data acquisition success rate of 93%. The analysis identified 2419 gene alterations, with a median of 11 alterations per tumor (range, 0–86). The most common or likely pathogenic variants were on TP53, TERT, PI3KCA, CDKN2A/B, KRAS, CCDN1, FGF19, FGF3, and SMAD4. The median tumor mutation burden was three mutations/Mb (range, 0–117) in 143 patients with available data. Of 150 patients with known or likely pathogenic actionable alterations, 13 (8.6%) received matched targeted therapy. Sixty-nine patients underwent Molecular Tumor Board, which resulted in recommendations in 60 cases. Treatment with genotype-directed therapy had no impact on overall survival (13 months vs. 14 months; p = 0.95; hazard ratio = 1.04 (95% confidence interval, 0.48–2.26)].ConclusionsThis study highlights that an organized center with a Multidisciplinary Molecular Tumor Board and an NGS screening system can obtain satisfactory results comparable with those of large centers for including patients in clinical trials.

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Section: Discussionsupporting

confidence: 90%

Section: Discussionsupporting

confidence: 90%

Clinical management of molecular alterations identified by high throughput sequencing in patients with advanced solid tumors in treatment failure: Real-world data from a French hospital

et al. 2023

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“…Although comprehensive genomic profiling using cancer gene panels has demonstrated value in broadening the treatment options for the patients based on matching a patient’s genomic lesions to cancer driver gene aberrations associated with FDA-approved treatment indications 8,9 , the presence/absence of mutations in such genes does not necessarily translate into improved predictive power for estimating the patient’s response to the potential treatments. While for some drugs, the variation in drug response can be explained by a very specific mutation, for instance, BRAF V600E mutation is a strong predictor for response to Vemurafenib in metastatic melanoma 4 , for many drugs, the knowledge of the mechanism of action is missing.…”

Section: Mainmentioning

confidence: 99%

Multi-omics alleviates the limitations of panel-sequencing for cancer drug response prediction

Baranovskii

Gunduz

Franke

et al. 2022

Preprint

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Comprehensive genomic profiling using cancer gene panels has been shown to improve treatment options for a variety of cancer types. However, genomic aberrations detected via such gene panels don't necessarily serve as strong predictors of drug sensitivity. In this study, using pharmacogenomics datasets of cell lines, patient-derived xenografts, and ex-vivo treated fresh tumor specimens, we demonstrate that utilizing the transcriptome on top of gene panel features substantially improves drug response prediction performance in cancer.

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“…41 Another study using a different CGP test (FoundationOne), which has both liquid biopsy-and tissue biopsy-based assays, reported a cost of $4,700 per sample in 2021. 42 In the US, certain commercially available CGP tests require blood samples to be sent to central laboratories for analysis, and the results are reported to the donor's health care provider. One of these tests (Guardant360) costs US$5,000 for people paying out-of-pocket.…”

Section: Costmentioning

confidence: 99%

An Overview of Comprehensive Genomic Profiling Technologies to Inform Cancer Care

Basharat¹,

Farah²

2022

cjht

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Horizon Scan reports provide brief summaries of information regarding new and emerging health technologies; Heath Technology Update articles typically focus on a single device or intervention. This Horizon Scan summarizes the available information regarding emerging comprehensive genomic profiling (CGP) technologies for informing cancer treatments. These technologies are based on next-generation sequencing platforms, which can characterize up to hundreds of genes and other genomic information with a single sample. Emerging tests are also compatible with minimally invasive liquid biopsies that use fluids such as blood samples to support clinical decision-making. CGP could be an alternative or a complement to conventional testing that uses single-biomarker assays or limited gene panels. Some emerging CGP tests available in Canada, the US, and Europe are being considered to inform the treatment of non–small cell lung cancer (NSCLC) because it has the highest number of identified biomarkers. Most identified studies have examined CGP use with NSCLC. The emerging evidence about the clinical and cost-effectiveness of CGP technologies for either NSCLC or other cancer types remains uncertain. Without randomized trials and robust study designs, it is not yet well-established whether the additional costs and technical requirements of CGP may provide better clinical outcomes compared with conventional molecular testing. This Horizon Scan also provides considerations for health systems about testing infrastructure, training for health care professionals, and understanding different patients’ perspectives should CGP or other next-generation sequencing technologies become more widely used in Canada.

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The Impact of Foundation Medicine Testing on Cancer Patients: A Single Academic Centre Experience

Cited by 12 publications

References 22 publications

Clinical management of molecular alterations identified by high throughput sequencing in patients with advanced solid tumors in treatment failure: Real-world data from a French hospital

Clinical management of molecular alterations identified by high throughput sequencing in patients with advanced solid tumors in treatment failure: Real-world data from a French hospital

Multi-omics alleviates the limitations of panel-sequencing for cancer drug response prediction

An Overview of Comprehensive Genomic Profiling Technologies to Inform Cancer Care

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