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壶腹癌中279个癌症基因的测序揭示了与组织学亚型相关的趋势以及ERBB2(HER2)的频繁扩增和过表达。

Sequencing of 279 cancer genes in ampullary carcinoma reveals trends relating to histologic subtypes and frequent amplification and overexpression of ERBB2 (HER2).

作者信息

Hechtman Jaclyn F, Liu Weiguo, Sadowska Justyna, Zhen Lisa, Borsu Laetitia, Arcila Maria E, Won Helen H, Shah Ronak H, Berger Michael F, Vakiani Efsevia, Shia Jinru, Klimstra David S

机构信息

Department of Pathology, Memorial Sloan Kettering Cancer Center, New York, NY, USA.

Department of Pathology, University of Buffalo, Buffalo, NY, USA.

出版信息

Mod Pathol. 2015 Aug;28(8):1123-9. doi: 10.1038/modpathol.2015.57. Epub 2015 May 15.

Abstract

The biological relevance of histological subtyping of ampullary carcinoma into intestinal vs pancreaticobiliary types remains to be determined. In an effort to molecularly profile these subtypes of ampullary carcinomas, we conducted a two-phase study. In the discovery phase, we identified 18 pancreatobiliary-type ampullary carcinomas and 14 intestinal-type ampullary carcinomas using stringent pathologic criteria and performed next-generation sequencing targeting 279 cancer-associated genes on these tumors. Although the results showed overlapping of genomic alterations between the two subtypes, trends including more frequent KRAS alterations in pancreatobiliary-type ampullary carcinoma (61 vs 29%) and more frequent mutations in APC in intestinal-type ampullary carcinoma (43 vs 17%) were observed. Of the entire cohort of 32 tumors, the most frequently mutated gene was TP53 (n=17); the most frequently amplified gene was ERBB2 (n=5); and the most frequently deleted gene was CDKN2A (n=6). In the second phase of the study, we aimed at validating our observation on ERBB2 and assessed ERBB2 amplification and protein overexpression in a series of 100 ampullary carcinomas. We found that (1) gene amplification and immunohistochemical overexpression of ERBB2 occurred in 13% of all ampullary carcinomas, therefore providing a potential target for anti-HER2 therapy in these tumors; (2) amplification and immunohistochemical expression correlated in all cases, thus indicating that immunohistochemistry could be used to screen tumors; and (3) none of the 14 ERBB2-amplified tumors harbored any downstream driver mutations in KRAS/NRAS, whereas 56% of the cases negative for ERBB2 amplification did, an observation clinically pertinent as downstream mutations may cause primary resistance to inhibition of EGFR family members.

摘要

壶腹癌组织学亚型分为肠型和胰胆管型的生物学相关性仍有待确定。为了从分子层面剖析这些壶腹癌亚型,我们开展了一项两阶段研究。在发现阶段,我们运用严格的病理标准,鉴定出18例胰胆管型壶腹癌和14例肠型壶腹癌,并对这些肿瘤中279个与癌症相关的基因进行了二代测序。尽管结果显示这两种亚型之间存在基因组改变的重叠,但仍观察到一些趋势,包括胰胆管型壶腹癌中KRAS改变更为频繁(61% 对29%),以及肠型壶腹癌中APC突变更为频繁(43% 对17%)。在全部32例肿瘤中,最常发生突变的基因是TP53(n = 17);最常扩增的基因是ERBB2(n = 5);最常缺失的基因是CDKN2A(n = 6)。在研究的第二阶段,我们旨在验证对ERBB2的观察结果,并评估了100例壶腹癌中ERBB2的扩增和蛋白过表达情况。我们发现:(1)13%的所有壶腹癌中出现了ERBB2基因扩增和免疫组化过表达,因此为这些肿瘤的抗HER2治疗提供了一个潜在靶点;(2)扩增与免疫组化表达在所有病例中均相关,这表明免疫组化可用于筛查肿瘤;(3)14例ERBB2扩增的肿瘤中,无一例在KRAS/NRAS中有任何下游驱动突变,而ERBB2扩增阴性的病例中有56%存在下游突变,这一观察结果具有临床相关性,因为下游突变可能导致对EGFR家族成员抑制的原发性耐药。

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