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全面分析、免疫和虫草素对泛癌及配对健康组织中 SOX9 表达的调控作用。

Comprehensive analysis, immune, and cordycepin regulation for SOX9 expression in pan-cancers and the matched healthy tissues.

机构信息

Key Laboratory of Epigenetics and Oncology, Research Center for Preclinical Medicine, Southwest Medical University, Luzhou, China.

Department of Obstetrics, The Affiliated Hospital of Southwest Medical University, Luzhou, China.

出版信息

Front Immunol. 2023 Mar 20;14:1149986. doi: 10.3389/fimmu.2023.1149986. eCollection 2023.

Abstract

SRY-box transcription factor 9 (SOX9) (OMIM 608160) is a transcription factor. The expression of SOX9 in pan-cancers and the regulation by small molecules in cancer cell lines are unclear. In the current study, we comprehensively analyzed the expression of SOX9 in normal tissues, tumor tissues and their matched healthy tissues in pan-cancers. The study examined the correlation between immunomodulators and immune cell infiltrations in normal and tumor tissues. Cordycepin (CD), an adenosine analog for SOX9 expression regulation, was also conducted on cancer cells. The results found that SOX9 protein is expressed in a variety of organs, including high expression in 13 organs and no expression in only two organs; in 44 tissues, there was high expression in 31 tissues, medium expression in four tissues, low expression in two tissues, and no expression in the other seven tissues. In pan-cancers with 33 cancer types, SOX9 expression was significantly increased in fifteen cancers, including CESC, COAD, ESCA, GBM, KIRP, LGG, LIHC, LUSC, OV, PAAD, READ, STAD, THYM, UCES, and UCS, but significantly decreased in only two cancers (SKCM and TGCT) compared with the matched healthy tissues. It suggests that SOX9 expression is upregulated in the most cancer types (15/33) as a proto-oncogene. The fact that the decrease of SOX9 expression in SKCM and the increase of SOX9 in the cell lines of melanoma inhibit tumorigenicity in both mouse and human models demonstrates that SOX9 could also be a tumor suppressor. Further analyzing the prognostic values for SOX9 expression in cancer individuals revealed that OS is long in ACC and short in LGG, CESC, and THYM, suggesting that high SOX9 expression is positively correlated with the worst OS in LGG, CESC, and THYM, which could be used as a prognostic maker. In addition, CD inhibited both protein and mRNA expressions of SOX9 in a dose-dependent manner in 22RV1, PC3, and H1975 cells, indicating CD's anticancer roles likely SOX9 inhibition. Moreover, SOX9 might play an important role in tumor genesis and development by participating in immune infiltration. Altogether, SOX9 could be a biomarker for diagnostics and prognostics for pan-cancers and an emerging target for the development of anticancer drugs.

摘要

性别决定区 Y 框转录因子 9(SOX9)(OMIM 608160)是一种转录因子。SOX9 在泛癌中的表达以及在癌细胞系中受小分子的调控尚不清楚。在本研究中,我们全面分析了 SOX9 在泛癌中的正常组织、肿瘤组织及其配对健康组织中的表达。研究还检测了免疫调节剂与正常和肿瘤组织中免疫细胞浸润的相关性。我们还研究了虫草素(CD)对 SOX9 表达调控的作用,CD 是一种腺苷类似物,可用于癌症细胞。结果发现,SOX9 蛋白在多种器官中表达,在 13 种器官中高表达,在仅 2 种器官中不表达;在 44 种组织中,有 31 种组织高表达,4 种组织中表达中等,2 种组织中表达低,7 种组织中不表达。在具有 33 种癌症类型的泛癌中,与配对的健康组织相比,SOX9 在 15 种癌症(CESC、COAD、ESCA、GBM、KIRP、LGG、LIHC、LUSC、OV、PAAD、READ、STAD、THYM、UCES 和 UCS)中表达显著增加,但在仅两种癌症(SKCM 和 TGCT)中表达显著降低。这表明 SOX9 表达作为原癌基因在上皮癌中上调(15/33)。SKCM 中 SOX9 表达降低和黑色素瘤细胞系中 SOX9 增加抑制了两者在小鼠和人类模型中的致瘤性,这表明 SOX9 也可能是一种肿瘤抑制因子。进一步分析癌症个体中 SOX9 表达的预后价值表明,ACC 的 OS 较长,LGG、CESC 和 THYM 的 OS 较短,提示高 SOX9 表达与 LGG、CESC 和 THYM 中最差的 OS 呈正相关,可作为预后标志物。此外,CD 以剂量依赖的方式抑制 22RV1、PC3 和 H1975 细胞中 SOX9 的蛋白和 mRNA 表达,表明 CD 的抗癌作用可能与 SOX9 抑制有关。此外,SOX9 可能通过参与免疫浸润在肿瘤发生和发展中发挥重要作用。总的来说,SOX9 可能成为泛癌的诊断和预后标志物,也是开发抗癌药物的新靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b283/10067558/1dcb848750e9/fimmu-14-1149986-g001.jpg

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