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对匹配的局部和转移性原发性高危 SCC 进行靶向下一代测序,可鉴定出驱动突变和共同发生的突变以及新的治疗靶点。

Targeted next-generation sequencing of matched localized and metastatic primary high-risk SCCs identifies driver and co-occurring mutations and novel therapeutic targets.

机构信息

Department of Dermatology, University of Nebraska Medical Center, Omaha, NE, United States.

Department of Dermatology, University of Nebraska Medical Center, Omaha, NE, United States; University of Southern California Keck School of Medicine, Los Angeles, CA, United States.

出版信息

J Dermatol Sci. 2020 Jul;99(1):30-43. doi: 10.1016/j.jdermsci.2020.05.007. Epub 2020 May 29.

DOI:10.1016/j.jdermsci.2020.05.007
PMID:32595073
Abstract

BACKGROUND

Cutaneous squamous cell carcinoma (SCC) is the second most common type of skin cancer and is responsible for over one million cases annually. While only 3-5 % of SCCs metastasize, those that do are associated with significant morbidity and mortality. Using gene mutations to help predict metastasis and select therapeutics is still being explored.

OBJECTIVE

To present novel data from targeted sequencing of 20 case-matched localized and metastatic high-risk SCCs.

METHODS

A cancer-associated gene panel of 76 genes was run from formalin-fixed paraffin-embedded samples of 20 case-matched localized (10) and metastatic (10) high-risk SCCs (Vela Diagnostics).

RESULTS

Using spatial clustering analysis, primary driver mutations were identified asEGFR in localized SCC and CDH1 in metastatic SCC. ERBB4 and STK11 were found to be significant co-occurring mutations in localized SCC. Pathway analyses showed the RTK/RAS, TP53, TGF-b, NOTCH1, PI3K, and cell cycle pathways to be highly relevant in all high-risk SCCs with the Wnt pathway enhanced in metastatic SCC only.

CONCLUSIONS

This study compared gene mutations between localized and metastatic SCC with the intent of identifying key differences and new potential targeted treatment options. To our knowledge, the co-occurrence ofERBB4 and STK11 mutations has not been previously reported. Targeted inhibition of CDH1 and the Wnt pathway should be further explored in metastatic SCC.

摘要

背景

皮肤鳞状细胞癌(SCC)是第二常见的皮肤癌类型,每年导致超过 100 万例病例。虽然只有 3-5%的 SCC 发生转移,但那些转移的 SCC 与显著的发病率和死亡率相关。利用基因突变来帮助预测转移并选择治疗方法仍在探索之中。

目的

展示 20 例匹配的局部和转移性高危 SCC 靶向测序的新数据。

方法

对 20 例匹配的局部(10 例)和转移性(10 例)高危 SCC(Vela Diagnostics)的福尔马林固定石蜡包埋样本进行了 76 个基因的癌症相关基因panel 检测。

结果

通过空间聚类分析,确定了局部 SCC 中的 EGFR 和转移性 SCC 中的 CDH1 为主要驱动突变。在局部 SCC 中发现 ERBB4 和 STK11 是显著共同发生的突变。通路分析显示 RTK/RAS、TP53、TGF-b、NOTCH1、PI3K 和细胞周期通路在所有高危 SCC 中均高度相关,而 Wnt 通路仅在转移性 SCC 中增强。

结论

本研究比较了局部 SCC 和转移性 SCC 之间的基因突变,旨在确定关键差异和新的潜在靶向治疗选择。据我们所知,ERBB4 和 STK11 突变的共同发生以前没有报道过。CDH1 和 Wnt 通路的靶向抑制应在转移性 SCC 中进一步探索。

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