探讨丝氨酸-精氨酸丰富的剪接因子：口腔癌失调的潜在预测标志物。

Exploring serine-arginine rich splicing factors: potential predictive markers for dysregulation in oral cancer.

机构信息

Dr. B. R. Ambedkar Centre for Biomedical Research (ACBR), University of Delhi, Delhi, 110007, India.

Bai Jerbai Wadia Hospital for Children, Parel, Mumbai, 400014, Maharashtra, India.

出版信息

BMC Cancer. 2024 Sep 3;24(1):1094. doi: 10.1186/s12885-024-12750-4.

DOI:10.1186/s12885-024-12750-4

PMID:39227899

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11373262/

Abstract

BACKGROUND

Dysregulated splicing events are a common phenomenon in cancer with the Serine-arginine-rich splicing factor (SRSF) family emerging as pivotal regulators of gene expression, exerting influence over constitutive and alternative splicing processes. Although aberrations in a few SRSF family members have been implicated in various cancers, the comprehensive roles of other family constituents remain underexplored.

METHODS

This study delves into the expression profile of the entire SRSF family (SRSF1-SRSF12) in 23 cancerous cell lines originating from diverse tissues using quantitative Real-Time PCR. Further, the transcript levels of the SRSF family were examined in oral cancer patient samples stratified into Pre-cancer (n = 15), Early cancer (n = 11), Late cancer (n = 14), and adjacent non-tumor tissues (n = 26) as controls. The results were corroborated by a parallel investigation utilizing the transcriptomics data of oral squamous cell carcinoma (OSCC) patients (n = 319) and controls (n = 35) available in The Cancer Genome Atlas (TCGA) database.

RESULTS

Our investigation reveals a notable upregulation in the expression levels of key splicing factors, namely SRSF3, SRSF9, and SRSF10 in all oral cancer cell lines (SCC-4, UM-SCC-84, CAL33, SAS-H1). Conversely, no significant associations between SRSF family members and other cancer cell lines were discerned. Further, the expression profile of the SRSF family in oral cancer patient samples revealed significant upregulation of SRSF1, SRSF3, SRSF7, SRSF9, SRSF10, and SRSF11 in patients with late-stage oral cancer compared to controls. Transcriptomics data from TCGA database demonstrated remarkable upregulation of SRSF1, SRSF4, SRSF9, SRSF10, and SRSF11 in OSCC patients.

CONCLUSION

Collectively our results underscore the critical involvement of SRSF family members in the context of oral cancer, highlighting their potential as key players in the altered splicing dynamics associated with cancer progression.

摘要

背景

剪接事件失调是癌症的一种常见现象，丝氨酸/精氨酸丰富的剪接因子（SRSF）家族作为基因表达的关键调节剂而出现，对组成性和选择性剪接过程都有影响。尽管少数 SRSF 家族成员的异常与各种癌症有关，但其他家族成分的全面作用仍未得到充分探索。

方法

本研究使用定量实时 PCR 研究了来自不同组织的 23 种癌细胞系中整个 SRSF 家族（SRSF1-SRSF12）的表达谱。此外，还检查了口腔癌患者样本中 SRSF 家族的转录水平，这些患者分为癌前病变（n=15）、早期癌症（n=11）、晚期癌症（n=14）和相邻非肿瘤组织（n=26）作为对照。这一结果得到了使用来自癌症基因组图谱（TCGA）数据库的口腔鳞状细胞癌（OSCC）患者（n=319）和对照（n=35）的转录组学数据进行的平行研究的证实。

结果

我们的研究表明，关键剪接因子 SRSF3、SRSF9 和 SRSF10 的表达水平在所有口腔癌细胞系（SCC-4、UM-SCC-84、CAL33、SAS-H1）中均显著上调。相反，在其他癌细胞系中没有发现 SRSF 家族成员之间的显著相关性。此外，口腔癌患者样本中的 SRSF 家族表达谱显示，与对照组相比，晚期口腔癌患者 SRSF1、SRSF3、SRSF7、SRSF9、SRSF10 和 SRSF11 的表达显著上调。TCGA 数据库的转录组学数据显示，OSCC 患者的 SRSF1、SRSF4、SRSF9、SRSF10 和 SRSF11 显著上调。