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High‐resolution genomic alterations in Barrett's metaplasia of patients who progress to esophageal dysplasia and adenocarcinoma

FHIT公司 CDKN2A 发育不良 肠化生 化生 腺癌 癌症研究 生物 食管 食道疾病 胃肠病学 内科学 医学 肿瘤科 癌症 癌变 抑癌基因
作者
Jorge L. Sepulveda,Elena V. Komissarova,Sarawut Kongkarnka,Richard A. Friedman,Jon M. Davison,Brynn Levy,Diana Bryk,Vaidehi Jobanputra,Armando Del Portillo,Gary W. Falk,Joshua Sonett,Charles J. Lightdale,Julian A. Abrams,Timothy C. Wang,Antonia R. Sepulveda
出处
期刊:International Journal of Cancer [Wiley]
卷期号:145 (10): 2754-2766 被引量:11
标识
DOI:10.1002/ijc.32351
摘要

The main risk factor for esophageal dysplasia and adenocarcinoma (DAC) is Barrett's esophagus (BE), characterized by intestinal metaplasia. The critical genomic mechanisms that lead to progression of nondysplastic BE to DAC remain poorly understood and require analyses of longitudinal patient cohorts and high‐resolution assays. We tested BE tissues from 74 patients, including 42 nonprogressors from two separate groups of 21 patients each and 32 progressors (16 in a longitudinal cohort before DAC/preprogression‐BE and 16 with temporally concurrent but spatially separate DAC/concurrent‐BE). We interrogated genome‐wide somatic copy number alterations (SCNAs) at the exon level with high‐resolution SNP arrays in DNA from formalin‐fixed samples histologically confirmed as nondysplastic BE. The most frequent abnormalities were SCNAs involving FHIT exon 5, CDKN2A/B or both in 88% longitudinal BE progressors to DAC vs . 24% in both nonprogressor groups ( p = 0.0004). Deletions in other genomic regions were found in 56% of preprogression‐BE but only in one nonprogressor‐BE ( p = 0.0004). SCNAs involving FHIT exon 5 and CDKN2A/B were also frequently detected in BE temporally concurrent with DAC. TP53 losses were detected in concurrent‐BE but not earlier in preprogression‐BE tissues of patients who developed DAC. CDKN2A/p16 immunohistochemistry showed significant loss of expression in BE of progressors vs . nonprogressors, supporting the genomic data. Our data suggest a role for CDKN2A/B and FHIT in early progression of BE to dysplasia and adenocarcinoma that warrants future mechanistic research. Alterations in CDKN2A/B and FHIT by high‐resolution assays may serve as biomarkers of increased risk of progression to DAC when detected in BE tissues.

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