Flow cytometric DNA analysis and p53 protein expression show a good correlation with histologic findings in patients with barrett's esophagus

Giménez, A; Minguela, Alfredo; Parrilla, Pascual; Bermejo, Juan; Pérez, Domingo; Molina, Joaquín; García, A. Fernández; Ortiz, M. Ángeles; Álvarez, Rocío; Haro, L. Martinez De

doi:10.1002/(sici)1097-0142(19980815)83:4<641::aid-cncr3>3.0.co;2-n

Cited by 50 publications

(18 citation statements)

References 54 publications

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“…p53 was a more powerful predictor of progression than LGD (RR 4.5 vs 2.4), but the two combined yielded a relative risk of 11.2. Importantly, in the Gimenez study 53 indefinite for dysplasia showing p53-positivity was much more likely to progress than if negative (5/7 vs 1/10). In Kaye et al 9 status of this group was not specifically provided but, currently, of LGD and ID cases which had sufficient material for p53 staining and follow up, 14/20 p53-positives progressed vs 3/12 p53-negatives (unpublished data).…”

Section: P53 As a Predictor Of Progression In Barrett'ssupporting

confidence: 67%

p53 Immunohistochemistry as a biomarker of dysplasia and neoplastic progression in Barrett's oesophagus

Kaye

2015

Diagnostic Histopathology

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Section: P53 As a Predictor Of Progression In Barrett'ssupporting

confidence: 67%

p53 Immunohistochemistry as a biomarker of dysplasia and neoplastic progression in Barrett's oesophagus

Kaye

2015

Diagnostic Histopathology

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“…This is probably due to the purity of our cell population obtained by selection of specific cells by LCM, and direct sequencing of PCR products in both directions, rather than using indirect techniques. 7,12,15,16,18,[23][24][25][26][27][28][29] Therefore, the role of p53 mutation as a prognostic factor in progression of metaplastic BE toward esophageal adenocarcinoma is not certain. Since the molecular basis of p53 function and mutations is not fully understood, a better evaluation of the biological properties of different p53 mutations is needed in order to interpret the results.…”

Section: Discussionmentioning

confidence: 90%

Evaluation of p53 mutations in premalignant esophageal lesions and esophageal adenocarcinoma using laser capture microdissection

et al. 2004

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p53 mutations have been implicated in the development of esophageal malignancies. The purpose of this study was to assess more accurately the incidence and types of p53 mutations in Barrett's esophagus (BE) with and without dysplasia and in esophageal adenocarcinoma, using pure preparations of epithelial cells obtained by laser capture microdissection (LCM). Assays were performed on paraffin-embedded tissue samples of normal antrum and premalignant and malignant esophageal samples from 57 patients, including 16 controls, 10 with BE metaplasia alone, 20 with BE-associated dysplasia, and 11 with BE-associated adenocarcinoma. All tissues were processed for LCM. DNA was extracted from isolated cells, and polymerase chain reaction (PCR) was performed using oligonucleutide primers for exons 5-8 of p53. PCR products were processed for DNA sequencing. p53 sequence abnormalities were identified in 2/16 cases of normal antrum and regenerative/ chemical gastritis, 1/10 cases of BE, 1/20 cases of BE with dysplasia, and 2/11 cases of adenocarcinomas. The abnormalities occurred in exons 7 and 8 in the form of point mutations. Our results, using LCM, show that p53 gene mutations are relatively rare in esophageal preneoplastic and neoplastic conditions. Only point mutations were detected, but no deletions/insertions were identified.

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“…The evolution of clones that we report here is also consistent with neoplasia, and recognition of BE as a benign neoplasm may improve our understanding of the basis for its precancerous potential. The study of evolution requires measurement of changes in allele frequencies, and we did not assess the relationship between genotypes and dysplastic phenotypes because the two were generated on different samples that could not be directly compared quantitatively, although the relationships among p16, p53, and cytometric abnormalities and dysplasia have been published previously by us and others (2,17,18,25,69,(82)(83)(84)(85)(86).…”

Section: Markermentioning

confidence: 99%

Selectively Advantageous Mutations and Hitchhikers in Neoplasms

et al. 2004

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Neoplastic progression is an evolutionary process characterized by genomic instability and waves of clonal expansions carrying genetic and epigenetic lesions to fixation (100% of the cell population). However, an evolutionarily neutral lesion may also reach fixation if it spreads as a hitchhiker on a selective sweep. We sought to distinguish advantageous lesions from hitchhikers in the premalignant condition Barrett's esophagus. Patients (211) had biopsies taken at 2-cm intervals in their Barrett's segments. Purified epithelial cells were assayed for loss of heterozygosity and microsatellite shifts on chromosomes 9 and 17, sequence mutations in CDKN2A/MTS1/INK4a (p16) and TP53 (p53), and methylation of the p16 promoter. We measured the expanse of a lesion in a Barrett's segment as the proportion of proliferating cells that carried a lesion in that locus. We then selected the lesion having expanses >90% in the greatest number of patients as our first putative advantageous lesion. We filtered out hitchhikers by removing all expanses of other lesions that did not occur independent of the advantageous lesion. The entire process was repeated on the remaining expanses to identify additional advantageous lesions. p16 loss of heterozygosity, promoter methylation, and sequence mutations have strong, independent, advantageous effects on Barrett's cells early in progression. Second lesions in p16 and p53 are associated with later selective sweeps. Virtually all of the other lesion expansions, including microsatellite shifts, could be explained as hitchhikers on p16 lesion clonal expansions. These techniques can be applied to any neoplasm.

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Flow cytometric DNA analysis and p53 protein expression show a good correlation with histologic findings in patients with barrett's esophagus

Cited by 50 publications

References 54 publications

p53 Immunohistochemistry as a biomarker of dysplasia and neoplastic progression in Barrett's oesophagus

p53 Immunohistochemistry as a biomarker of dysplasia and neoplastic progression in Barrett's oesophagus

Evaluation of p53 mutations in premalignant esophageal lesions and esophageal adenocarcinoma using laser capture microdissection

Selectively Advantageous Mutations and Hitchhikers in Neoplasms

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