Validation of a Plasma-Based Comprehensive Cancer Genotyping Assay Utilizing Orthogonal Tissue- and Plasma-Based Methodologies

Odegaard, Justin I.; Vincent, John J.; Mortimer, Stefanie; Vowles, James V.; Ulrich, Bryan C.; Banks, Kimberly C.; Fairclough, Stephen R.; Zill, Oliver A.; Sikora, Marcin; Mokhtari, Reza; Abdueva, Diana; Nagy, Rebecca J.; Lee, Christine E.; Kiedrowski, Lesli A.; Paweletz, Cloud P.; Eltoukhy, Helmy; Lanman, Richard B.; Chudova, Darya; Talasaz, AmirAli

doi:10.1158/1078-0432.ccr-17-3831

Cited by 314 publications

(295 citation statements)

References 51 publications

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“…This is the largest reported cohort to-date describing the genomic landscape of advanced-stage METex14-mutated NSCLC. We evaluated the frequency with which METex14 mutations co-occur with other cancer-associated mutations ( Supplemental Table 1) (11,15). Synonymous mutations and those with predicted neutral or unknown functional impact were excluded, as previously described (11), as were mutations previously associated with clonal hematopoiesis (16).…”

Section: Co-occurring Genomic Alterations Are Common In Advanced-stagmentioning

confidence: 99%

Co-occurring alterations in the RAS-MAPK pathway limit response to MET inhibitor treatment inMETexon 14 skipping mutation positive lung cancer

Rotow

Gui

et al. 2018

Preprint

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Abstract:While patients with advanced-stage non-small cell lung cancers (NSCLCs) harboring MET exon 14 skipping mutations (METex14) often benefit from MET tyrosine kinase inhibitor (TKI) treatment, their long-term survival is limited by drug resistance. The molecular basis for this resistance remains incompletely understood. Through targeted sequencing analysis of cell-free circulating tumor DNA obtained from 289 patients with advanced-stage METex14 NSCLC, we find prominent co-occurring RAS pathway gene alterations (e.g. in KRAS/NRAS, NF1). Clinical resistance to MET TKI treatment was associated with the presence of these co-occurring alterations. In a new preclinical model expressing a METex14 mutation, KRAS overexpression promoted MET TKI resistance, which was overcome by co-treatment with crizotinib and the MEK inhibitor trametinib. Our study provides a genetic landscape of co-occurring alterations in advanced-stage METex14-mutated NSCLC and suggests a potential combination therapy strategy to enhance clinical outcomes. Statement of Significance:This report describes targeted sequencing of the largest reported cohort of advanced-stage NSCLC with a MET exon 14 skipping mutation. The data uncover certain RAS pathway genetic alterations as potential mediators of MEK TKI resistance, which could be overcome by MEK and MET co-inhibition in NSCLC.Introduction:

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Section: Co-occurring Genomic Alterations Are Common In Advanced-stagmentioning

confidence: 99%

Co-occurring alterations in the RAS-MAPK pathway limit response to MET inhibitor treatment inMETexon 14 skipping mutation positive lung cancer

Rotow

Gui

et al. 2018

Preprint

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“…Plasma is a well‐known liquid biopsy for analyzing the genetic status of tumors . However, the abundance of cell‐free tumor DNA in plasma is low, and therefore it is possible that mutations may not be detected in early‐stage cancer.…”

Section: Discussionmentioning

confidence: 99%

“…Plasma is a well-known liquid biopsy for analyzing the genetic status of tumors. 15,29 However, the abundance of cell-free tumor DNA in plasma is low, and therefore it is possible that mutations may not be detected in early-stage cancer. We previously showed that the concentration of cell-free tumor DNA is diluted from proximal to distal sites from tumor lesions.…”

Section: Discussionmentioning

confidence: 99%

Genomic profile of urine has high diagnostic sensitivity compared to cytology in non‐invasive urothelial bladder cancer

et al. 2019

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Cytology is widely conducted for diagnosis of urothelial bladder cancer; however, its sensitivity is still low. Recent studies show that liquid biopsies can reflect tumor genomic profiles. We aim to investigate whether plasma or urine is more suitable for detecting tumor‐derived DNA in patients with early‐stage urothelial bladder cancer. Targeted sequencing of 71 genes was carried out using a total of 150 samples including primary tumor, urine supernatant, urine precipitation, plasma and buffy coat from 25 patients with bladder cancer and five patients with cystitis and benign tumor. We compared mutation profiles between each sample, identified tumor‐identical mutations and compared tumor diagnostic sensitivities between urine and conventional cytology. We identified a total of 168 somatic mutations in primary tumor. In liquid biopsies, tumor‐identical mutations were found at 53% (89/168) in urine supernatant, 48% (81/168) in urine precipitation and 2% (3/168) in plasma. The high variant allele fraction of urine was significantly related to worse clinical indicators such as tumor invasion and cytological examination. Although conventional cytology detected tumor cells in only 22% of non‐invasive tumor, tumor diagnostic sensitivity increased to 67% and 78% using urine supernatant and precipitation, respectively. Urine is an ideal liquid biopsy for detecting tumor‐derived DNA and more precisely reflects tumor mutational profiles than plasma. Genomic analysis of urine is clinically useful for diagnosis of superficial bladder cancer at early stage.

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“…NGS analysis of cfDNA from peripheral blood is effective to capture comprehensive genomic information of tumor cells when tissue genotyping is infeasible or insufficient in metastatic disease . Targeted cfDNA NGS testing enables detection of low‐frequency somatic mutations with high sensitivity due to low tumor shedding . Currently, cfDNA sequencing has been applied in many cancer types to identify oncogenic aberrations.…”

Section: Introductionmentioning

confidence: 99%

“…16 Targeted cfDNA NGS testing enables detection of low-frequency somatic mutations with high sensitivity due to low tumor shedding. 17 Currently, cfDNA sequencing has been applied in many cancer types to identify oncogenic aberrations. Despite dramatic changes in technology, a large knowledge deficit remains in the clinical value of fluid biopsy for LAM subjects.…”

Section: Introductionmentioning

confidence: 99%

Identification of driver genes and somatic mutations in cell‐free DNA of patients with pulmonary lymphangioleiomyomatosis

Zhang

Wang

et al. 2019

Intl Journal of Cancer

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Next‐generation sequencing of cell‐free circulating DNA (cfDNA) has emerged as promising technique for identifying minimally invasive genomic profiling of tumor cells recently. However, it remains relatively unknown in LAM disease. In our study, paired cfDNA and genomic DNA (gDNA) in blood samples were obtained from 23 LAM patients and seven healthy controls to explore mutations profiles of targeted 70 cancer‐related genes. As results, log2‐based allele frequencies of mutations in cfDNA were significantly different from those of gDNA. By comparing the mutual mutations identified both in cfDNA and gDNA, a significant correlation was also observed. After removing mutations in gDNA, distinct somatic mutation profiles of cfDNA were observed in LAM patients. Forty of 70 targeted genes had recurrent mutations, of which ATM, BRCA2 and APC showed the highest frequency. Based on the mutation, correlation network constructed of 40 mutated genes, 11 hub genes bearing intensive interactions were highlighted, including BRCA1, BRCA2, RAD50, RB1, NF1, APC, MLH3, ATM, PDGFRA, PALB2 and BLM. Expression of the hub genes showed significant clusters between LAM patients and controls and that RAD50 and BRCA2 had the strongest associations with subject phenotypes. Myogenesis and estrogen response were confirmed to be positively regulated in LAM patients. Collectively, our study provided a landscape of genomic alterations in LAM and discovered several potential driver genes, that is, BRCA2 and RAD50, which shed a substantial light on the clinical application of key molecular markers and potential therapy targets for precision diagnosis and treatment in the future.

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Validation of a Plasma-Based Comprehensive Cancer Genotyping Assay Utilizing Orthogonal Tissue- and Plasma-Based Methodologies

Cited by 314 publications

References 51 publications

Co-occurring alterations in the RAS-MAPK pathway limit response to MET inhibitor treatment inMETexon 14 skipping mutation positive lung cancer

Co-occurring alterations in the RAS-MAPK pathway limit response to MET inhibitor treatment inMETexon 14 skipping mutation positive lung cancer

Genomic profile of urine has high diagnostic sensitivity compared to cytology in non‐invasive urothelial bladder cancer

Identification of driver genes and somatic mutations in cell‐free DNA of patients with pulmonary lymphangioleiomyomatosis

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