SMARCA4 和 SMARCE1 在胃癌中的表达：与 ARID1A、微卫星不稳定性的相关性，以及 SMARCE1/ERBB2 共扩增。

SMARCA4 and SMARCE1 in gastric cancer: Correlation with ARID1A, and microsatellite stability, and SMARCE1/ERBB2 co-amplification.

机构信息

Department of Pathology, Christian-Albrechts-University, University-Hospital Schleswig-Holstein, Kiel, Germany.

Department of Internal Medicine II, Christian-Albrechts-University, University-Hospital Schleswig-Holstein, Kiel, Germany.

出版信息

Cancer Med. 2023 May;12(9):10423-10437. doi: 10.1002/cam4.5776. Epub 2023 Mar 14.

DOI:10.1002/cam4.5776

PMID:36916408

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10225191/

Abstract

BACKGROUND

Recent studies have shown an association between certain subunits of the SWI/SNF complex with specific tumor characteristics in gastric cancer (GC). In an earlier study, we applied multiregional whole exome sequencing on multiple primary tumor samples and found alterations of the SWI/SNF complex in 78% of the cases. ERBB2, which encodes for Her2/neu, is a well-known predictive biomarker used to guide the treatment of GC in the palliative setting. SMARCE1, which encodes for a subunit of the SWI/SNF complex, is localized in close genetic proximity to ERBB2.

AIM

As little is known about the significance of the SWI/SNF complex in GC biology and the potential relationship between ERBB2 and SMARCE1 upregulation, we examined the expression patterns of SMARCA4 and SMARCE1, two mutually exclusive catalytic ATPase subunits of the SWI/SNF complex, in a well characterized GC cohort.

MATERIALS AND METHODS

The expression of SMARCA4 and SMARCE1 was studied by immunohistochemistry in connection with clinicopathological patient characteristics in a cohort of 468 GCs. Digital droplet polymerase chain reaction was performed for amplification analysis on ERBB2 and SMARCE1.

RESULTS

Immunohistochemical staining of whole-mount tissue sections found a diffusely "gray scale" expression of SMARCA4 in 446 (95.2%) GCs and of SMARCE1 in 463 (98.8%) GCs. The expression of SMARCA4 and SMARCE1 correlated significantly with ARID1A, p53, and microsatellite status. No correlation was found with the patient prognosis. The amplification analysis of SMARCE1 showed amplification in 4 of 34 cases. In 3 of 34 cases, SMARCE1 was co-amplified with ERBB2. We also found a co-expression of SMARCE1 and Her2/neu in a subset of patients.

CONCLUSION

While the effect of a co-amplification is currently unknown, synergistic effects of SMARCE1 and Her2/neu overexpression should be explored in future studies, holding potential for an improved treatment of GC.

摘要

背景

最近的研究表明，SWI/SNF 复合物的某些亚基与胃癌（GC）的特定肿瘤特征有关。在早期的一项研究中，我们对多个原发性肿瘤样本进行了多区域全外显子测序，发现 78%的病例存在 SWI/SNF 复合物的改变。编码 Her2/neu 的 ERBB2 是一种众所周知的预测性生物标志物，用于指导 GC 的姑息治疗。SMARCE1 编码 SWI/SNF 复合物的一个亚基，其定位于 ERBB2 的紧密遗传邻近位置。

目的

由于对 SWI/SNF 复合物在 GC 生物学中的意义以及 ERBB2 和 SMARCE1 上调之间的潜在关系知之甚少，我们在一个具有良好特征的 GC 队列中检查了 SWI/SNF 复合物的两个相互排斥的催化 ATP 酶亚基 SMARCA4 和 SMARCE1 的表达模式。

材料和方法

我们对 468 例 GC 患者的临床病理特征进行了免疫组织化学研究，以研究 SMARCA4 和 SMARCE1 的表达情况。我们对 ERBB2 和 SMARCE1 进行了数字液滴聚合酶链反应（PCR）扩增分析。

结果

对全组织切片的免疫组织化学染色发现，446 例（95.2%）GC 中 SMARCA4 呈弥漫性“灰度”表达，463 例（98.8%）GC 中 SMARCE1 呈弥漫性“灰度”表达。SMARCA4 和 SMARCE1 的表达与 ARID1A、p53 和微卫星状态显著相关。与患者预后无相关性。SMARCE1 的扩增分析显示，34 例中有 4 例扩增。在 34 例中，SMARCE1 与 ERBB2 共扩增。我们还在一组患者中发现了 SMARCE1 和 Her2/neu 的共表达。

结论

虽然目前尚不清楚共扩增的影响，但应在未来的研究中探索 SMARCE1 和 Her2/neu 过表达的协同作用，为 GC 的治疗提供新的思路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6c47/10225191/25e7f2b3d8b8/CAM4-12-10423-g004.jpg

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SMARCA4 和 SMARCE1 在胃癌中的表达：与 ARID1A、微卫星不稳定性的相关性，以及 SMARCE1/ERBB2 共扩增。

SMARCA4 and SMARCE1 in gastric cancer: Correlation with ARID1A, and microsatellite stability, and SMARCE1/ERBB2 co-amplification.

机构信息

出版信息

BACKGROUND

AIM

MATERIALS AND METHODS

RESULTS

CONCLUSION

背景

目的

材料和方法

结果

结论

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