非肌层浸润性膀胱癌的基因组亚型:指导暴露于马兜铃酸的患者的免疫治疗决策
Genomic subtypes of non-muscle-invasive bladder cancer: guiding immunotherapy decision-making for patients exposed to aristolochic acid.
作者信息
Peng Yun, Song Yuxuan, Qin Caipeng, Ding Mengting, Huang Zixiong, Wang Fei, HuangFu Yuchao, Yu Luping, Du Yiqing, Xu Tao
机构信息
Department of Urology, Peking University People's Hospital, Beijing, 100044, China.
出版信息
Mol Med. 2025 Apr 17;31(1):140. doi: 10.1186/s10020-025-01199-1.
BACKGROUND
The limited genomic data on non-muscle-invasive bladder cancer (NMIBC) hampers our understanding of its carcinogenesis and development. Specifically, Aristolochic acid (AA), a potent human carcinogenic compound from aristolochia plants and commonly found in Chinese herbal medicine, has been extensively documented as being closely associated with the onset and progression of bladder cancer. However, the field of AA-induced NMIBC remains largely unexplored in terms of its genomic and molecular characteristics, as well as clinical therapeutic strategies.
METHODS
To bridge this knowledge gap, we conducted a comprehensive study using a cohort of 81 NMIBC samples. We performed whole-exome sequencing (WES) and RNA sequencing (RNA-seq) to obtain detailed genomic and transcriptomic data. We subjected these datasets to genomic analysis and subtype analysis to gain valuable insights into NMIBC.
RESULTS
By temporally dissecting mutations in NMIBC specimens, we identified a comprehensive mutational landscape of NMIBC and the associations of these mutations with recurrence-free survival. Additionally, we discerned four genomic subtypes of NMIBC: AA-like, FGFR3/HRAS, FGFR3 & chr9Del, and genome instability (GI). The AA-like subtype presented a high frequency of gene mutations along with a pronounced AA mutagenesis signature of SBS22 (Fisher test: P-value 3.5e-4, OR 25.25) even after temporal dissection. The FGFR3/HRAS subtype exhibited FGFR3 or HRAS mutations with few copy number alterations (CNAs). The FGFR3 & chr9Del subtype was characterized by the co-occurrence of chr9p and chr9q deletions as well as FGFR3 mutations, while the GI subtype showed a high frequency of CNAs. Notably, the AA-like and GI subtypes demonstrated better outcomes after immunotherapy, whereas the FGFR3/HRAS subtype showed poorer outcomes.
CONCLUSIONS
Our findings provide novel perspectives on the genomics of NMIBC, unveiling four prominent genomic subtypes, each showing different outcomes following immunotherapy.
TRIAL REGISTRATION
No. 2019PHB268-01 (retrospectively registered on February 14, 2020).
背景
非肌层浸润性膀胱癌(NMIBC)的基因组数据有限,这阻碍了我们对其致癌机制和发展过程的理解。具体而言,马兜铃酸(AA)是一种源自马兜铃属植物的强效人类致癌化合物,常见于中草药中,已有大量文献记载其与膀胱癌的发生和进展密切相关。然而,在AA诱导的NMIBC的基因组和分子特征以及临床治疗策略方面,该领域仍 largely未被探索。
方法
为填补这一知识空白,我们使用81例NMIBC样本队列进行了一项全面研究。我们进行了全外显子测序(WES)和RNA测序(RNA-seq)以获得详细的基因组和转录组数据。我们对这些数据集进行基因组分析和亚型分析,以深入了解NMIBC。
结果
通过对NMIBC标本中的突变进行时间剖析,我们确定了NMIBC的全面突变图谱以及这些突变与无复发生存率的关联。此外,我们识别出NMIBC的四种基因组亚型:AA样、FGFR3/HRAS、FGFR3 & chr9Del和基因组不稳定(GI)。即使在时间剖析后,AA样亚型仍呈现出高频率的基因突变以及明显的SBS22的AA诱变特征(Fisher检验:P值3.5e-4,OR 25.25)。FGFR3/HRAS亚型表现出FGFR3或HRAS突变,拷贝数改变(CNA)较少。FGFR3 & chr9Del亚型的特征是chr9p和chr9q缺失以及FGFR3突变同时出现,而GI亚型显示出高频率CNA。值得注意的是,AA样和GI亚型在免疫治疗后显示出更好的结果,而FGFR3/HRAS亚型显示出较差的结果。
结论
我们的研究结果为NMIBC的基因组学提供了新的视角,揭示了四种突出的基因组亚型,每种亚型在免疫治疗后显示出不同的结果。
试验注册
第2019PHB268-01号(于2020年2月14日追溯注册)。
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