Epithelial dysplasia of the stomach with gastric immunophenotype shows features of biological aggressiveness

Valente, Pedro; Garrido, Mónica; Gullo, Irene; Baldaia, Helena; Marques, Margarida; Baldaque‐Silva, Francisco; Lopes, Joanne; Carneiro, Fátima

doi:10.1007/s10120-014-0416-5

Cited by 34 publications

(36 citation statements)

References 29 publications

(33 reference statements)

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“…Several authors have found differential genetic and epigenetic alterations in gastric versus intestinal phenotypes [50,51], although the association with specific clinicopathological features and the prognosis is still conflicting [45,51]. During GC progression, a phenotypic switch may occur from gastric to intestinal differentiation [45]; moreover, some authors hypothesise that GC with a gastric phenotype may also progress to poorly differentiated GC [44,47].…”

Section: Morphological Heterogeneity Of Gcmentioning

confidence: 99%

“…According to their expression, four GC immunophenotypes have been recognised: the intestinal (expressing MUC2, CD10, CDX2), gastric (expressing MUC5AC/TTF1 and/ or MUC6/TTF2), hybrid (expressing intestinal and gastric markers), and null phenotype [43][44][45][46]. These phenotypes have also been recognised in GC precursor lesions [47][48][49]. Several authors have found differential genetic and epigenetic alterations in gastric versus intestinal phenotypes [50,51], although the association with specific clinicopathological features and the prognosis is still conflicting [45,51].…”

Section: Morphological Heterogeneity Of Gcmentioning

confidence: 99%

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Heterogeneity in Gastric Cancer: From Pure Morphology to Molecular Classifications

Gullo

Carneiro²,

Oliveira³

et al. 2017

Pathobiology

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108

103

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Gastric cancer (GC) represents a global health concern. Despite advances in prevention, diagnosis, and therapy, GC is still the third leading cause of cancer mortality worldwide, with more than 720,000 estimated deaths in 2012. Overall survival for advanced disease is about 1 year, a dismal prognosis that is partly due to the high levels of biological heterogeneity found in GC. Indeed, GC is a highly heterogeneous disease from morphological and molecular standpoints. The numerous histological and molecular classifications currently available reflect such heterogeneity. Although recent high-throughput studies cluster the molecular data obtained into subgroups with clinical relevance, we still need a practical, prognostic, and predictive classification system, integrating morphological and molecular features, towards the identification of novel therapeutic targets. It is noteworthy that GC heterogeneity encompasses not only interpatient variability (intertumour heterogeneity), but also variations within the same tumour (intratumour heterogeneity). The latter encompasses spatial heterogeneity (in different tumour areas) and temporal heterogeneity (along progression from primary to recurrent and/or metastatic disease). In this review, we analyse the morphological, immunophenotypic, and molecular heterogeneity in GC as the basis for a better understanding of the disease, and discuss the practical implications for diagnostic pathology, prognostic evaluation, and precision therapy.

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Section: Morphological Heterogeneity Of Gcmentioning

confidence: 99%

Section: Morphological Heterogeneity Of Gcmentioning

confidence: 99%

Heterogeneity in Gastric Cancer: From Pure Morphology to Molecular Classifications

Gullo

Carneiro²,

Oliveira³

et al. 2017

Pathobiology

Self Cite

108

103

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show abstract

“…Despite a considerable decrease in the incidence of gastric cancer (GC) in many developed countries, GC remains the fourth most commonly diagnosed malignancy and the second leading cause of cancer-related death worldwide [1,2]. In the past few decades, standard multimodal treatment strategies have been used to improve outcomes in patients with GC, particularly those with advanced and metastatic diseases [2].…”

Section: Introductionmentioning

confidence: 99%

Genetic differences stratified by PCR-based microsatellite analysis in gastric intramucosal neoplasia

et al. 2016

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Background Although genetic alterations in patients with advanced gastric cancer have been extensively studied, those in patients with intramucosal neoplasia (IMN) are still poorly understood. Methods We evaluated genetic differences in 158 IMNs, including 51 low-grade dysplasias, 58 high-grade dysplasias (HGDs), 30 intramucosal cancers (IMCs), and 19 mixed tumors (composed of IMC and HGD within the same tumor), using PCR-based microsatellite analysis [allelic imbalance (AI) and microsatellite instability (MSI)]. We classified the DNA methylation status as a hypermethylated epigenome, a moderately methylated epigenome, or a hypomethylated epigenome. In addition, p53 overexpression, b-catenin nuclear localization, and mucin expression were also examined. Results From cluster analysis, the IMNs examined were categorized into four subgroups as follows. Tumors in subgroup 1 were characterized by MSI-high status, a hypermethylated epigenome, and loss or reduction of expression of MLH-1. Tumors in subgroup 2 showed a mixed pattern consisting of AI and MSI. In contrast, tumors in subgroup 3, which showed accumulation of multiple AIs, were closely associated with HGD, IMC, or mixed tumor and exhibited nuclear expression of b-catenin. Tumors in subgroup 4, which were generally low-grade dysplasias, exhibited a low frequency of AIs and no MSI. Although the mucin phenotype was not correlated with any subgroup, expression of mucin was associated with some subgroups. Overexpression of p53 was common in all subgroups. Conclusion The approach described herein was useful for studying genetic differences in IMNs. In addition, we suggest that stratification of genetic differences may help to identify genetic molecular profiles in IMNs.

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“…It has been suggested that this variant originates in the native or non-metaplastic gastric mucosa, rather than in intestinal metaplastic lesions with the involvement of spasmolytic polypeptide-expressing metaplasia (SPEM) pathway of carcinogenesis. 40 There are no validated criteria for morphologically establishing a hybrid phenotype (with both adenomatous and gastric differentiation). In such instances, the immunohistochemical expression of MUC proteins (MUC2, MUC5AC and MUC6), CDX2, and CD10 have been used to establish the mixed lineage.…”

Section: Phenotype Based Risk Of Carcinomamentioning

confidence: 99%

Gastric dysplasia: update and practical approach

Setia¹,

Lauwers²

2015

Diagnostic Histopathology

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Epithelial dysplasia of the stomach with gastric immunophenotype shows features of biological aggressiveness

Cited by 34 publications

References 29 publications

Heterogeneity in Gastric Cancer: From Pure Morphology to Molecular Classifications

Heterogeneity in Gastric Cancer: From Pure Morphology to Molecular Classifications

Genetic differences stratified by PCR-based microsatellite analysis in gastric intramucosal neoplasia

Gastric dysplasia: update and practical approach

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