整合单细胞和大量 RNA 测序数据,发现 RBM17 是膀胱癌免疫疗法的新型反应生物标记物。

IF 3.4 3区 医学 Q1 PATHOLOGY
Bo Song, Peishan Wu, Chong Wan, Qiangqiang Sun, Guangqi Kong
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引用次数: 0

摘要

检查点抑制剂(CPIs)已被广泛应用于膀胱癌(BLCA)患者的治疗。然而,对反应预测生物标志物的研究仍处于起步阶段。为了发现癌细胞中与 CPI 反应相关的标记基因,我们利用 SCISSOR 整合了单细胞 RNA 和大容量 RNA 测序数据。我们收集了来自 IMvigor210、UNC-108 和 BCAN/HCRN 数据集的转录组和临床数据,以评估和验证已确定的生物标记和特征。此外,我们还分析了 TCGA-BLCA 和 local-BLCA RNA-seq 数据,以研究替代剪接事件(ASE)。我们评估了RBM17上调或下调的T24和UMUC3细胞的存活率。通过 SCISSOR 分析,我们发现 RBM17、TAP1 和 PSMB8 的表达水平与 CPI 反应显著相关。由于 PSMB8 与 TAP1 呈高度正相关,我们根据 RBM17 和 TAP1 的表达谱建立了 CPI 反应评分(CRS)特征。CRS在IMvigor210、UNC-108和BCAN/HCRN数据集中表现出强大的预测能力,并与较高的肿瘤突变负荷(TMB)、PD-L1表达和独特的基因组特征相关。值得注意的是,RBM17 与 BLCA 患者的临床结果无关,但与 BLCA 细胞的体外增殖呈正相关。同时,RBM17与核心生物通路的较高活性相关,包括抗原处理机制、CD8 + T效应细胞、细胞周期、DNA损伤修复、上皮-间质转化、组蛋白调控和免疫检查点。此外,高RBM17组显示出LumU/Ba/sq亚型的富集,但FGFR3改变较少。最后,RBM17明显上调了BLCA样本中的ASE,导致新抗原水平升高、肿瘤微环境更加炎症以及CPI反应改善。RBM17与较高的ASEs和新抗原水平相关,从而增强了CPI对BLCA的疗效。仅利用两个基因就建立起的预测特征具有简化临床应用的潜力,为昂贵的基因组、转录组和生物特征测试提供了一种具有成本效益的替代方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Integrating single cell and bulk RNA sequencing data identifies RBM17 as a novel response biomarker for immunotherapy in bladder cancer.

Checkpoint inhibitors (CPIs) have been widely applied in the treatment of patients with bladder cancer (BLCA). However, there is still unmet need to dissect response predict biomarkers. To uncover CPI response-related marker genes in cancer cells, we utilized SCISSOR, integrating single-cell RNA and bulk RNA sequencing data. Transcriptomic and clinical data from IMvigor210, UNC-108, and BCAN/HCRN datasets were collected to evaluate and validate the identified biomarkers and signatures. Additionally, we analyzed TCGA-BLCA and local-BLCA RNA-seq data to investigate alternative splicing events (ASEs). Cell viability was assessed in T24 and UMUC3 cells with RBM17 upregulation or downregulation. Through SCISSOR analysis, we discovered that the expression levels of RBM17, TAP1, and PSMB8 were significantly associated with CPI response. Since PSMB8 displayed a highly positive correlation with TAP1, we developed a CPI response score (CRS) signature based on the expression profiles of RBM17 and TAP1. The CRS demonstrated robust predictive capacity in IMvigor210, UNC-108, and BCAN/HCRN datasets and was associated with higher tumor mutational burden (TMB), PD-L1 expression, and unique genomic features. Notably, RBM17 was not linked to the clinical outcomes of BLCA patients but positively correlated with BLCA cell proliferation in vitro. In the meantime, RBM17 was correlated with higher activity in core biological pathways, including antigen processing machinery, CD8 + T effector cells, cell cycle, DNA damage repair, epithelial-mesenchymal transition, histone regulation, and immune checkpoints. Moreover, the high-RBM17 group showed enrichment of LumU/Ba/sq subtypes but fewer FGFR3 alterations. Lastly, RBM17 significantly upregulated ASEs in BLCA samples, leading to higher neoantigen levels, a more inflamed tumor microenvironment, and improved CPI response. RBM17 is associated with higher ASEs and neoantigen levels, thereby potentiating the efficacy of CPI in BLCA. The established predictive signature, utilizing only two genes, has the potential to streamline clinical applications, providing a cost-effective alternative to expensive genomic, transcriptomic, and biological feature tests.

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来源期刊
Virchows Archiv
Virchows Archiv 医学-病理学
CiteScore
7.40
自引率
2.90%
发文量
204
审稿时长
4-8 weeks
期刊介绍: Manuscripts of original studies reinforcing the evidence base of modern diagnostic pathology, using immunocytochemical, molecular and ultrastructural techniques, will be welcomed. In addition, papers on critical evaluation of diagnostic criteria but also broadsheets and guidelines with a solid evidence base will be considered. Consideration will also be given to reports of work in other fields relevant to the understanding of human pathology as well as manuscripts on the application of new methods and techniques in pathology. Submission of purely experimental articles is discouraged but manuscripts on experimental work applicable to diagnostic pathology are welcomed. Biomarker studies are welcomed but need to abide by strict rules (e.g. REMARK) of adequate sample size and relevant marker choice. Single marker studies on limited patient series without validated application will as a rule not be considered. Case reports will only be considered when they provide substantial new information with an impact on understanding disease or diagnostic practice.
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