Longitudinal tracking of 97 esophageal adenocarcinomas using liquid biopsy sampling

Ococks, Emma; Frankell, Alexander M.; Soler, N. Masque; Grehan, Nicola; Northrop, A.; Coles, H. M. T.; Redmond, Aisling M.; Devonshire, Ginny; Weaver, Jamie; Hughes, Craig D.; Lehovsky, Katie; Blasko, Adrienn; Nutzinger, Barbara; Fitzgerald, Rebecca C.; Smyth, Elizabeth

doi:10.1016/j.annonc.2020.12.010

Cited by 73 publications

(101 citation statements)

References 32 publications

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“…When analyzing the 31 samples collected postsurgery, we demonstrated that 70% of patients with a FrEIA score above the detection threshold (13 out of 18 patients) developed a recurrence. Our results are comparable to mutation-based detection of tumor-derived cfDNA in resectable EAC (7,8). In a recent publication a ctDNA panel consisting of 77 genes was tested in 97 EAC patients.…”

Section: Discussionsupporting

confidence: 72%

“…In a recent publication a ctDNA panel consisting of 77 genes was tested in 97 EAC patients. After filtering of CHIP variants, the panel showed high prognostic potential for disease-free survival (HR 5.35, 95% CI 2.10-13.63; P ≤ 0.0001) based on the post-surgery samples (7). Another paper used an EAC tumor guided sequencing approach and found ctDNA status (positive vs. negative) to be prognostic at baseline for disease-free survival (p=0.042) (8).…”

Section: Discussionmentioning

confidence: 99%

“…To evaluate the prognostic value of FrEIA in a clinical setting, we tested cfDNA from resectable EAC patients, where serial ctDNA detection has been shown to predict adverse outcome (7). Here we assessed the potential of the FrEIA score in 293 resectable EAC samples from 2 clinical cohorts: a neoadjuvant chemoradiotherapy (nCRT) cohort (n=70 patients, n = 149 plasma samples) receiving standard of care carboplatin combined with paclitaxel based nCRT and a cohort of patients who participated in the phase II PERFECT trial (n=40 patients, n = 144 samples, see Methods) received nCRT in combination with a PD-L1 inhibitor (27).…”

Section: Prognostic Potential Of Fres and Freia Scorementioning

confidence: 99%

“…Mutation-based detection of tumor-derived cfDNA is often hampered by technical and biological noise (the latter linked to the accumulation of mutations in normal cells) (5,6). For example, in elderly patients with TP53 mutant tumors, such as in esophageal adenocarcinoma (EAC), clonal hematopoiesis of indeterminate potential (CHIP) hampers the determination of the origin of cfDNA variants (6,7). In stage I-III patients with a low tumor fraction of cfDNA this requires a high sequencing depth for cfDNA, availability of buffy coat samples, tumor-informed sequencing or computational strategies to filter CHIP-derived variants (8,9).…”

Section: Introductionmentioning

confidence: 99%

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Genome-wide cell-free DNA termini in patients with cancer

Moldován

Pol

Ende

et al. 2021

Preprint

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The structure, fragmentation pattern, length and terminal sequence of cell-free DNA (cfDNA) is under the influence of nucleases present in the blood. We hypothesized that differences in the diversity of bases at the end of cfDNA fragments can be leveraged on a genome-wide scale to enhance the sensitivity for detecting the presence of tumor signals in plasma. We surveyed the cfDNA termini in 572 plasma samples from 319 patients with 18 different cancer types using low-coverage whole genome sequencing. The fragment-end sequence and diversity were altered in all cancer types in comparison to 76 healthy controls. We converted the fragment end sequences into a quantitative metric and observed that this correlates with circulating tumor DNA tumor fraction (R = 0.58, p < 0.001, Spearman). Using these metrics, we were able to classify cancer samples from control at a low tumor content (AUROC of 91% at 1% tumor fraction) and shallow sequencing coverage (mean AUROC = 0.99 at >1M fragments). Combining fragment-end sequences and diversity using machine learning, we classified cancer from healthy controls (mean AUROC = 0.99, SD = 0.01). Using unsupervised clustering we showed that early-stage lung cancer (n = 13) can be classified from control or later stages based on fragment-end sequences. We observed that fragment-end sequences can be used for prognostication (hazard ratio: 0.49) and residual disease detection in resectable esophageal adenocarcinoma patients, moving fragmentomics toward a greater clinical implementation.

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Section: Discussionsupporting

confidence: 72%

Section: Discussionmentioning

confidence: 99%

Section: Prognostic Potential Of Fres and Freia Scorementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Genome-wide cell-free DNA termini in patients with cancer

Moldován

Pol

Ende

et al. 2021

Preprint

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“…Of note, growing evidence suggests a higher benefit of ICB-therapies in circulating tumor DNA (ctDNA)-positive patients in several malignancies, with a favorable prognostic role of ctDNA seroconversion rates ( 177 ) ( 178 ). Consolidated data concerning eventual prognostic/predictive roles of this biomarker could possibly instruct for the use of ctDNA seroconversion rate as a primary endpoint of (neo)adjuvant CV clinical trials, alongside long-term survival data (i.e.…”

Section: Introductionmentioning

confidence: 99%

Therapeutic cancer vaccines revamping: technology advancements and pitfalls

et al. 2021

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Cancer vaccines (CVs) represent a long-sought therapeutic and prophylactic immunotherapy strategy to obtain antigen-specific T-cell responses, and potentially achieve long-term clinical benefit. However, historically, most CV clinical trials have resulted in disappointing outcomes, despite promising signs of immunogenicity across most formulations. In the past decade, technologic advances regarding vaccine delivery platforms, tools for immunogenomic profiling and antigen/epitope selection have occurred. Consequently, the ability of CVs to induce tumor-specific and, in some cases, remarkable clinical responses have been observed in early-phase clinical trials. It is notable that the record-breaking speed of vaccine development in response to the coronavirus disease (COVID-19) pandemic mainly relied on manufacturing infrastructures and technological platforms already developed for CVs. In turn, research, clinical data, and infrastructures put in place for the SARS-CoV2 pandemic can further speed CV development processes. This review outlines the main technological advancements as well as major issues to tackle in the development of CVs. Possible applications for unmet clinical needs will be described, putting into perspective the future of cancer vaccinology.

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Prognostic value of circulating tumour DNA during post‐radiotherapy surveillance in locally advanced esophageal squamous cell carcinoma

Wang

Cheng

et al. 2022

Clinical & Translational Med

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Background The potential of circulating tumour DNA (ctDNA) as a reliable biomarker for relapse/metastasis early detection and prognosis in esophageal squamous cell carcinoma (ESCC) after radiotherapy/chemoradiotherapy (RT/CRT) initiation requires comprehensive investigation. Methods Treatment‐naive locally advanced ESCC patients with available baseline plasma samples were prospectively enrolled from November 2018 to January 2020. RT/CRT was delivered with a simultaneous integrated boost of radiation dose. Serial plasma samples were collected at baseline (T0), week 4 of RT/CRT (T1), 1‐3 (T2) and 3‐6 months post‐RT/CRT (T3). ctDNA was analysed using next‐generation sequencing of 474 cancer‐relevant genes. Results A total of 128 plasma samples from 40 eligible patients were analysed (median age: 64 [range: 40‐78], 88% males, 95% stage III/IV), and the median follow‐up time was 20.6 months (range: 12.2‐33.3). During the post‐RT/CRT surveillance including 36 patients, radiological progression was observed in 16 patients, and 69% (11/16) had detectable post‐RT/CRT ctDNA prior to radiological progression, with a median lead time of 4.4 months compared with radiological imaging. ctDNA positivity at T1 (hazard ratio, HR: 3.60, 95% confidence interval, CI: 1.30‐10.01) or T2 (HR: 5.45, 95% CI: 1.72‐17.26) indicated inferior progression‐free survival (PFS). ctDNA clearance between T0‐T1 (HR: 0.31, 95% CI: 0.08‐1.13) or T0‐T2 (HR: 0.11; 95% CI: 0.02‐0.61) was associated with relatively favourable PFS. Similar results were obtained when focusing on patients without esophagectomy after RT/CRT. Notably, detectable ctDNA at T1 was a potential indicator of high local recurrence risks (HR: 4.43, 95% CI: 1.31‐15.04). Conclusions ctDNA was identified as a robust biomarker for early detection of disease progression and post‐RT/CRT prognosis stratification in ESCC. Detectable ctDNA at week 4 of RT/CRT might indicate higher local recurrence risks, implying the potential clinical utility of ctDNA tests in guiding post‐RT/CRT treatments for locoregional control in ESCC.

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Longitudinal tracking of 97 esophageal adenocarcinomas using liquid biopsy sampling

Cited by 73 publications

References 32 publications

Genome-wide cell-free DNA termini in patients with cancer

Genome-wide cell-free DNA termini in patients with cancer

Therapeutic cancer vaccines revamping: technology advancements and pitfalls

Prognostic value of circulating tumour DNA during post‐radiotherapy surveillance in locally advanced esophageal squamous cell carcinoma

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