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近端胃癌和胃食管交界腺癌异种移植中的一致性基因改变。

Consistent genetic alterations in xenografts of proximal stomach and gastro-esophageal junction adenocarcinomas.

作者信息

El-Rifai W, Harper J C, Cummings O W, Hyytinen E R, Frierson H F, Knuutila S, Powell S M

机构信息

Department of Medical Genetics, University of Helsinki, Finland.

出版信息

Cancer Res. 1998 Jan 1;58(1):34-7.

PMID:9426053
Abstract

The genetic alterations underlying the development of gastric and gastro-esophageal carcinoma remain largely undefined. DNA copy number changes were determined by comparative genomic hybridization in eight xenografts of proximal gastric and gastro-esophageal junction adenocarcinomas of the intestinal type. All tumors exhibited DNA copy number changes, with a total of 139 changes detected (range, 11-24 per tumor; mean = 17), indicating numerous and widespread alterations within these cancers. Gains (65%) in DNA copy number were more frequent than losses (35%). Our most striking finding was gain (all eight cases) or high-level amplification (four cases) in 20q, with a minimal common overlapping region at 20q13. Other frequent gains were observed at 6p, 7q, and 17q (six cases each) and at 1q, 2q, and 8q (five cases each). Frequent losses were observed at 4q and 5q (six cases each) and at 9p (five cases). No differences in DNA copy number changes were seen in tumors arising from the gastro-esophageal junction compared to those of the proximal stomach. The presence of common and consistent DNA copy number changes in these tumors implicate a number of chromosomal regions that may harbor important genes that are involved in tumorigenesis of the proximal stomach and gastro-esophageal junction.

摘要

胃癌和胃食管癌发生发展的潜在基因改变在很大程度上仍不明确。通过比较基因组杂交技术,对8例肠型近端胃癌和胃食管交界腺癌的异种移植瘤进行了DNA拷贝数变化检测。所有肿瘤均显示出DNA拷贝数变化,共检测到139处变化(范围为每个肿瘤11 - 24处;平均 = 17处),表明这些癌症中存在大量且广泛的改变。DNA拷贝数增加(65%)比减少(35%)更为常见。我们最显著的发现是20q出现增加(所有8例)或高水平扩增(4例),在20q13有一个最小的共同重叠区域。在6p、7q和17q(各6例)以及1q、2q和8q(各5例)也观察到其他常见的增加。在4q和5q(各6例)以及9p(5例)观察到常见的缺失。与近端胃的肿瘤相比,胃食管交界处产生的肿瘤在DNA拷贝数变化上未见差异。这些肿瘤中存在常见且一致的DNA拷贝数变化,提示一些染色体区域可能含有参与近端胃和胃食管交界肿瘤发生的重要基因。

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