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基于 SOX9 基因panel 的结直肠癌无创诊断

The non-invasive diagnosis of colorectal cancer via a SOX9-based gene panel.

机构信息

Department of Applied Biology and Chemical Technology, The Hong Kong Polytechnic University, Kowloon, Hong Kong Special Administrative Region, China.

Guangdong Provincial Key Laboratory of Regional Immunity and Diseases, International Cancer Center, Department of Pharmacology, Shenzhen University Health Science Center, Shenzhen, China.

出版信息

Clin Exp Med. 2023 Oct;23(6):2421-2432. doi: 10.1007/s10238-022-00970-6. Epub 2023 Jan 13.

Abstract

Colorectal cancer (CRC) threatens human health seriously. Early diagnosis of CRC is critical to improving patient survival. Meanwhile, non-invasive detection through tumor-circulating markers can be an important auxiliary diagnosis. In this study, we performed targeted RNA sequencing in paired tumor and adjacent normal fresh frozen tissues from 68 patients, and we also measured circulating mRNA levels in 4 time-point plasma samples collected before and after operation or chemotherapy. Our results showed that SOX9 (6.73-fold with adjusted p value < 1 × 10), MYC (20.59-fold with adjusted p value < 1 × 10), and MMP7 (131.94-fold with adjusted p value < 1 × 10) highly expressed in tumor compared with adjacent normal tissues. Besides, the circulating mRNA of SOX9 (41.14-fold with adjusted p value < 1 × 10) in CRC was significantly higher than in the normal control as well. Moreover, a SOX9-based 9-gene panel (SOX9, GSK3A, FZD4, LEF1, DVL1, FZD7, NFATC1, KRT19, and RUVBL1) showed the non-invasive diagnostic value of CRC (AUC: 0.863 (0.766-0.960), TPR: 0.92, TNR: 0.87). In summary, SOX9 expression consistently increases in tumor and plasma samples from CRC patients, which indicates the important role of SOX9 in CRC progression and its potential in non-invasive diagnosis of CRC.

摘要

结直肠癌(CRC)严重威胁人类健康。CRC 的早期诊断对于提高患者的生存率至关重要。同时,通过肿瘤循环标志物进行非侵入性检测可以作为重要的辅助诊断方法。在本研究中,我们对 68 例患者配对的肿瘤和相邻正常新鲜冷冻组织进行了靶向 RNA 测序,并在手术或化疗前后的 4 个时间点采集的血浆样本中测量了循环 mRNA 水平。我们的结果表明,SOX9(调整后的 p 值<1×10,6.73 倍)、MYC(调整后的 p 值<1×10,20.59 倍)和 MMP7(调整后的 p 值<1×10,131.94 倍)在肿瘤组织中高表达,与相邻的正常组织相比。此外,CRC 患者循环 SOX9 mRNA(调整后的 p 值<1×10,41.14 倍)也显著高于正常对照组。此外,基于 SOX9 的 9 基因组合(SOX9、GSK3A、FZD4、LEF1、DVL1、FZD7、NFATC1、KRT19 和 RUVBL1)显示了 CRC 的非侵入性诊断价值(AUC:0.863(0.766-0.960),TPR:0.92,TNR:0.87)。综上所述,SOX9 在 CRC 患者的肿瘤和血浆样本中持续表达增加,表明 SOX9 在 CRC 进展中的重要作用及其在 CRC 非侵入性诊断中的潜在应用。

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