Impact of Mutations in Subunit Genes of the Mammalian SWI/SNF Complex on Immunological Tumor Microenvironment.

IF 2.6 4区 医学 Q2 GENETICS & HEREDITY Cancer Genomics & Proteomics Pub Date : 2024-01-01 DOI:10.21873/cgp.20432
Chikako Hozumi, Akira Iizuka, Tomoatsu Ikeya, Haruo Miyata, Chie Maeda, Tadashi Ashizawa, Takeshi Nagashima, Kenichi Urakami, Yuji Shimoda, Keiichi Ohshima, Koji Muramatsu, Takashi Sugino, Akio Shiomi, Yasuhisa Ohde, Etsuro Bando, Kenichiro Furukawa, Teiichi Sugiura, Takashi Mukaigawa, Seiichiro Nishimura, Yasuyuki Hirashima, Koichi Mitsuya, Shusuke Yoshikawa, Yasuhiro Tsubosa, Hirohisa Katagiri, Masashi Niwakawa, Ken Yamaguchi, Hirotsugu Kenmotsu, Yasuto Akiyama
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Abstract

Background/aim: Recently, inactivating somatic mutations of SWI/SNF chromatin-remodeling genes in cancers have been reported. However, few studies have been performed regarding the immunological analysis of the tumor microenvironment (TME) in chromatin remodeling complex gene-mutated tumors. In the present study, we identified cancer patients harboring various mammalian SWI/SNF complex mutations and investigated the immunological features in those mutated cancers.

Patients and methods: Cancer patients harboring any type of chromatin remodeling complex gene mutation were selected and clinicopathological features were compared between chromatin remodeling complex gene expression-low and expression-high groups. Specifically, expression levels of immune response-associated genes and cancer-associated genes were compared between the SMARCA4 expression-low and expression-high groups using volcano plot analysis.

Results: Among cancers harboring PBRM1, SAMRACA4 and ARID2 gene mutations, T-cell marker and mature B-cell marker genes were up-regulated in the tumor. Specifically, T-cell effector genes (CD8B, CD40LG), central memory marker genes (CD27, CCR7) and mature B-cell marker genes (CD20, CD38, CD79 and IRF4) were up-regulated, and cancer-associated genes including MYB, MYC and AURKB genes were down-regulated in the SMARCA4 expression-low group. Remarkably, heatmap of gene expression and immunohistochemistry (IHC) data demonstrated that the tertiary lymphoid structure (TLS) gene signature of mature B cells was up-regulated in SMACA4 gene-mutated stomach cancers.

Conclusion: These results suggest that immune tumor microenvironment status, such as mature B cell recruitment featuring the TLS gene signature and immune activation mediated by cancer signal down-regulation, might contribute to the classification of SMARCA4 gene-mutated tumors as immune checkpoint blockade therapy-sensitive target tumors.

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哺乳动物 SWI/SNF 复合物亚基基因突变对免疫肿瘤微环境的影响
背景/目的:最近,有报道称癌症中的SWI/SNF染色质重塑基因发生了失活的体细胞突变。然而,有关染色质重塑复合基因突变肿瘤微环境(TME)免疫学分析的研究却很少。在本研究中,我们确定了携带各种哺乳动物SWI/SNF复合体突变的癌症患者,并调查了这些突变癌症的免疫学特征:筛选出携带任何一种染色质重塑复合体基因突变的癌症患者,并比较染色质重塑复合体基因表达量低和表达量高两组患者的临床病理特征。具体而言,采用火山图分析法比较了SMARCA4表达量低和表达量高两组之间免疫反应相关基因和癌症相关基因的表达水平:结果:在携带PBRM1、SAMRACA4和ARID2基因突变的癌症中,T细胞标记基因和成熟B细胞标记基因在肿瘤中上调。具体来说,T细胞效应基因(CD8B、CD40LG)、中央记忆标记基因(CD27、CCR7)和成熟B细胞标记基因(CD20、CD38、CD79和IRF4)在SMARCA4表达低的组中上调,而包括MYB、MYC和AURKB基因在内的癌症相关基因则下调。值得注意的是,基因表达和免疫组化(IHC)数据的热图显示,在SMARCA4基因突变的胃癌中,成熟B细胞的三级淋巴结构(TLS)基因特征被上调:这些结果表明,以TLS基因特征为特征的成熟B细胞募集和癌症信号下调介导的免疫激活等免疫肿瘤微环境状态可能有助于将SMARCA4基因突变的肿瘤划分为免疫检查点阻断疗法敏感的靶肿瘤。
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来源期刊
Cancer Genomics & Proteomics
Cancer Genomics & Proteomics ONCOLOGY-GENETICS & HEREDITY
CiteScore
5.00
自引率
8.00%
发文量
51
期刊介绍: Cancer Genomics & Proteomics (CGP) is an international peer-reviewed journal designed to publish rapidly high quality articles and reviews on the application of genomic and proteomic technology to basic, experimental and clinical cancer research. In this site you may find information concerning the editorial board, editorial policy, issue contents, subscriptions, submission of manuscripts and advertising. The first issue of CGP circulated in January 2004. Cancer Genomics & Proteomics is a journal of the International Institute of Anticancer Research. From January 2013 CGP is converted to an online-only open access journal. Cancer Genomics & Proteomics supports (a) the aims and the research projects of the INTERNATIONAL INSTITUTE OF ANTICANCER RESEARCH and (b) the organization of the INTERNATIONAL CONFERENCES OF ANTICANCER RESEARCH.
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