Extreme intratumour heterogeneity and driver evolution in mismatch repair deficient gastro-oesophageal cancer

Loga, Katharina von; Woolston, Andrew; Punta, Marco; Barber, Louise J.; Griffiths, Beatrice; Semiannikova, Maria; Spain, Georgia; Challoner, Benjamin; Fenwick, Kerry; Simon, Ronald; Marx, Andreas; Sauter, Guido; Lise, Stefano; Matthews, Nik; Gerlinger, Marco

doi:10.1038/s41467-019-13915-7

Cited by 51 publications

(67 citation statements)

References 76 publications

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“…Next, we generated multiregional trees based on driver SNVs and CNVs. As shown in Figure 1 all tumors of our cohort provided evidence of branched somatic evolution, with the most complex being the MSI GC, con rming data published recently by von Loga et al 7 In addition, we inferred maximum parsimony trees in accordance with Lee et al 5 (Suppl. Figure 4).…”

Section: Phylogenetic Analysissupporting

confidence: 88%

“…4 However, various validation studies conducted by ourselves and other research groups lead to the identi cation of a marked intratumoral heterogeneity, which stands to compromise the development and usage of targeted therapies in GC. 5,6,7 We found evidence of intratumoral heterogeneity for e.g. HER2 status, 8 MSI status 9 and PIK3CA genotype.…”

Section: Introductionmentioning

confidence: 63%

“…Among alterations in receptor tyrosine kinases, 9 of 12 cases (75%) were discordant across all matched samples. 6 Von Loga et al 7 recently studied four MSI GCs by multiregional sequencing and found an extreme intratumoral heterogeneity as well as evidence of parallel evolution in this special subtype of GC. Likewise, in our cohort of nine GCs, the vast majority of non-synonymous mutations was distributed "heterogeneously" and not present in each patient sample.…”

Section: Discussionmentioning

confidence: 99%

“…22 Multiregional sequencing studies provide evidence of somatic evolution shaping the genetic landscape of GC leading to a substantial intraprimary and intermetastatic heterogeneity. 5,6,7 However, while heterogeneity may shed some light on the subclonal architecture of the tumor, homogeneity does not necessarily represent clonality.…”

Section: Discussionmentioning

confidence: 99%

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Multiscale heterogeneity in gastric adenocarcinoma evolution is an obstacle to precision medicine

Röcken

Amallraja

Halske

et al. 2020

Preprint

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Background: Cancer is a somatic evolutionary disease, which adapts to environmental cues based on genetic constraints. Using multiregional exome sequencing, we tested the effect of somatic evolution on intratumoral heterogeneity and its putative clinical implications in adenocarcinomas of the stomach and gastroesophageal junction (GC). Methods: The study comprised a prospective discovery cohort of 9 and a validation cohort of 487 GCs. Multiregional whole-exome sequencing was done using 48 tumor samples (range: 3-10 tumor samples/patient) of the discovery cohort.Results: In total, the discovery cohort harbored 16,537 non-synonymous mutations (mutations/sample: median n=159; mutations/patient: median n=369). Intratumoral heterogeneity of somatic mutations and copy number variants were present in all tumors of the discovery cohort. 53-91% of the non-synonymous mutations were not present in each patient’s sample; 399 genes harbored 2-4 different non-synonymous mutations in the same patient; 175 genes showed copy number variations, the majority being heterogeneous, including CD274 (PD-L1). Phylogenetic analyses provided evidence for branched evolution being the most complex in a microsatellite instable GC. The analysis of the mode of evolution showed a high degree of heterogeneity in deviation from neutrality within each tumor. Studies on the validation cohort showed that the subclonal loss of SMAD4 is an independent predictor for poor patient outcome.Conclusions: Neutral and non-neutral somatic evolution shape the mutational landscape in GC. It leads to complex spatial intratumoral heterogeneity and may have profound effects on patient management. It provides crucial information for an individualized understanding of clinical prognosis and therapeutic options in GC patients.

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Section: Phylogenetic Analysissupporting

confidence: 88%

Section: Introductionmentioning

confidence: 63%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Multiscale heterogeneity in gastric adenocarcinoma evolution is an obstacle to precision medicine

Röcken

Amallraja

Halske

et al. 2020

Preprint

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“…Of note, MSI-H and PD-L1 POS phenotype are major prognostic factors as well as predictive biomarkers for ICI efficacy in GEC [21][22][23]. Multiregion exome sequencing revealed > 20-fold levels of intratumor heterogeneity in dMMR GEC compared to other cancer types, and also long phylogenetic trunks [24].…”

Section: Clinicopathologic and Molecular Features Of Mmr-deficient Gamentioning

confidence: 96%

Mismatch Repair System Genomic Scars in Gastroesophageal Cancers: Biology and Clinical Testing

Lopez

Venetis

Sajjadi

et al. 2020

Gastrointestinal Disorders

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Alterations in the mismatch repair (MMR) system result in genomic instability, neoantigen production, and immune response in cancer. There is evidence that gastroesophageal tumors with MMR deficiency may be susceptible to immune-checkpoint inhibitors treatment, especially in those presenting at advanced-stage disease. Although a number of biomarkers have been developed in histology-agnostic settings to assess MMR status, there is evidence that a tumor-specific testing approach would improve the selection of patients for immunotherapy. However, no testing methods have been developed specifically for gastroesophageal cancers so far. Here, we discuss the state of the art, current advances, and future perspectives of MMR-related biomarkers’ biologic and clinical role in gastroesophageal cancers.

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Tumor Heterogeneity

Maron

Bass

2020

JAMA Netw Open

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patients with heterogenous tumors to ascertain the spatial distribution of these potentially targetable copy number alterations. By evaluating multiple sites within 5 mm of each other, Chao et al uncovered heterogenous amplifications of MET, EGFR, FGFR2, and PIK3CA (OMIM 171834). Multisite FISH in these patients highlights how the initial computational approach underestimated the degree + Related articleAuthor affiliations and article information are listed at the end of this article.

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Extreme intratumour heterogeneity and driver evolution in mismatch repair deficient gastro-oesophageal cancer

Cited by 51 publications

References 76 publications

Multiscale heterogeneity in gastric adenocarcinoma evolution is an obstacle to precision medicine

Multiscale heterogeneity in gastric adenocarcinoma evolution is an obstacle to precision medicine

Mismatch Repair System Genomic Scars in Gastroesophageal Cancers: Biology and Clinical Testing

Tumor Heterogeneity

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