Differential clonal evolution in oesophageal cancers in response to neo-adjuvant chemotherapy

Findlay, John M.; Castro-Giner, Francesc; Makino, Seiko; Rayner, Emily; Kartsonaki, Christiana; Cross, William; Kováč, Michal; Ulahannan, Danny; Palles, Claire; Gillies, Richard; MacGregor, Thomas P.; Church, David N.; Maynard, Nicholas; Buffa, Francesca M.; Cazier, Jean‐Baptiste; Graham, Trevor A.; Wang, Lai-Mun; Sharma, Ricky A.; Middleton, Mark R.; Tomlinson, Ian

doi:10.1038/ncomms11111

Cited by 74 publications

(74 citation statements)

References 64 publications

(86 reference statements)

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“…Our study was performed as part of the ICGC, which is designed to examine the landscape by virtue of examining a large number of tumor:normal pairs, and hence, we were generally unable to perform multiregional sampling. Findlay et al (2016) recently reported results from their exome anlaysis of 30 preand post-chemotherapy EAC samples, and in this study, they purposefully selected cases showing a range of responses to chemotherapy. They associated good clinical response, as determined by the histopathological Mandard score generated from the post-chemotherapy surgical resection specimen, with evidence for genomic bottlenecking as a result of chemotherapy.…”

Section: Wwwgenomeorgmentioning

confidence: 99%

“…However, we also note they are two of the cases with the best pathological TNM staging. Any approach to prognosticate based on genomic factors (e.g., perhaps following the results of Findlay et al 2016) should at most temper established prognostic factors such as these fundamental phenotypic characteristics. Moreover, as discussed, some mutations were found to be more recurrent following chemotherapy, and this is an area ripe for further research as the appropriate cohorts become available.…”

Section: Wwwgenomeorgmentioning

confidence: 99%

“…We took the opportunity to critically evaluate the impact of chemotherapy on the genomic landscape. It has recently been reported from exome data that chemotherapy imposes a bottleneck on tumor evolution (Findlay et al 2016). We therefore first sought to establish the genetic relationship between 10 matched pre-and postchemotherapy samples and the point at which the samples diverged.…”

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A comparative analysis of whole genome sequencing of esophageal adenocarcinoma pre- and post-chemotherapy

et al. 2017

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The scientific community has avoided using tissue samples from patients that have been exposed to systemic chemotherapy to infer the genomic landscape of a given cancer. Esophageal adenocarcinoma is a heterogeneous, chemoresistant tumor for which the availability and size of pretreatment endoscopic samples are limiting. This study compares whole-genome sequencing data obtained from chemo-naive and chemo-treated samples. The quality of whole-genomic sequencing data is comparable across all samples regardless of chemotherapy status. Inclusion of samples collected post-chemotherapy increased the proportion of late-stage tumors. When comparing matched pre-and post-chemotherapy samples from 10 cases, the mutational signatures, copy number, and SNV mutational profiles reflect the expected heterogeneity in this disease. Analysis of SNVs in relation to allele-specific copy-number changes pinpoints the common ancestor to a point prior to chemotherapy. For cases in which pre-and post-chemotherapy samples do show substantial differences, the timing of the divergence is near-synchronous with endoreduplication. Comparison across a large prospective cohort (62 treatment-naive, 58 chemotherapy-treated samples) reveals no significant differences in the overall mutation rate, mutation signatures, specific recurrent point mutations, or copy-number events in respect to chemotherapy status. In conclusion, whole-genome sequencing of samples obtained following neoadjuvant chemotherapy is representative of the genomic landscape of esophageal adenocarcinoma. Excluding these samples reduces the material available for cataloging and introduces a bias toward the earlier stages of cancer.

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Section: Wwwgenomeorgmentioning

confidence: 99%

Section: Wwwgenomeorgmentioning

confidence: 99%

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confidence: 99%

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A comparative analysis of whole genome sequencing of esophageal adenocarcinoma pre- and post-chemotherapy

et al. 2017

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“…Shifting towards a focus on the underlying molecular and/or genetic mechanisms contributing to both response to therapy and longterm outcomes may add granularity to guide therapeutic decision making. Recent work has suggested genetic bottlenecking or intratumoral heterogeneity as potential markers for response to platinum-based therapy (20,21). In a study of 149 esophageal ACs potentially actionable gene alterations were identified in nearly half, while only one [ERBB2 (HER2)], is being routinely targeted (21).…”

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confidence: 99%

Adjuvant chemotherapy following trimodality therapy for esophageal carcinoma—Is the evidence sufficient?

2017

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“…These include highly complex molecular interactions in individual cancer cells (genetic, epigenetic, transcriptomic, proteomic), compounded by cellular interactions, tumour microenvironment, clonal heterogeneity, and tumour evolution during therapy (5). As a consequence, the effect sizes of these markers tend to be limited, and certainly an insufficient basis on which to decide whether to give or omit specific therapies (6).…”

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confidence: 99%

Challenges in assessing response of oesophageal cancer to neoadjuvant therapy, and the potential of composite PET-CT and multimodal metrics

Findlay¹,

Bradley²,

Gillies³

et al. 2017

J. Thorac. Dis.

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Differential clonal evolution in oesophageal cancers in response to neo-adjuvant chemotherapy

Cited by 74 publications

References 64 publications

A comparative analysis of whole genome sequencing of esophageal adenocarcinoma pre- and post-chemotherapy

A comparative analysis of whole genome sequencing of esophageal adenocarcinoma pre- and post-chemotherapy

Adjuvant chemotherapy following trimodality therapy for esophageal carcinoma—Is the evidence sufficient?

Challenges in assessing response of oesophageal cancer to neoadjuvant therapy, and the potential of composite PET-CT and multimodal metrics

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