膀胱肿瘤中几种常见APOBEC型突变的分析表明与病毒感染有关。

Nina Rao, Gabriel J Starrett, Mary L Piaskowski, Kelly E Butler, Yelena Golubeva, Wusheng Yan, Scott M Lawrence, Michael Dean, Montserrat Garcia-Closas, Dalsu Baris, Alison Johnson, Molly Schwenn, Nuria Malats, Francisco X Real, Manolis Kogevinas, Nathaniel Rothman, Debra T Silverman, Lars Dyrskjøt, Christopher B Buck, Stella Koutros, Ludmila Prokunina-Olsson
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引用次数: 0

摘要

FGFR3和PIK3CA是膀胱肿瘤中最常见的突变基因。我们假设这些基因的反复突变可能是由吸烟等常见致癌因素引起的。我们分析了2816例膀胱肿瘤,这些肿瘤具有FGFR3和/或PIK3CA突变的可用数据,重点是在≥10%的肿瘤中检测到的最复发的突变。与其他FGFR3/PIK3CA突变的肿瘤相比,FGFR3-Y375C在吸烟者的肿瘤中比从不吸烟者更常见(P=0.009),而几个APOBEC型驱动突变在从不吸烟者中富集:FGFR3-S249C(P=0.013)和PIK3CA-E542K/PIK3CA-E545K(P=0.009,我们分析了798例膀胱肿瘤的RNA测序(RNA-seq)数据,并检测到几种病毒,其中BK多瘤病毒(BKPyV)最常见。然后,我们在211个独立的膀胱肿瘤中对多瘤病毒(PyV)大T抗原(LTAg)进行了IHC染色。总的来说,通过RNA-seq或IHC-LTAg,我们在1010个膀胱肿瘤中的26个中检测到PyV,检测率显著更高(P=4.4×10-5),在非肌肉浸润性膀胱癌(NMIBC)中的554个中的25个(4.5%),而在肌肉浸润性囊癌(MIBC)中的456个中的1个(0.2%)。在NMIBC亚群中,在94.7%(18/19)的PyV阳性肿瘤中检测到FGFR3/PIK3CA APOBEC型驱动突变,而在68.3%(259/379)的PyV阴性肿瘤中(P=0.011)。在具有FGFR3-或PIK3CA突变肿瘤的NMIBC子群中,BKPyV肿瘤阳性也与更高的进展为MIBC的风险相关(P=0.019)。总之,我们的研究结果支持吸烟和BKPyV感染是通过不同的分子机制导致普通患者群体膀胱肿瘤发生的危险因素。预防相关性:吸烟可能导致膀胱肿瘤中最常见的突变之一(FGFR3-Y375C),而病毒感染可能导致其他三种突变(FGFR3-S249C、PIK3CA-E542K和PIK3CA-E645K)。了解这些突变的原因可能会导致新的预防和治疗策略,如病毒筛查和疫苗接种。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Analysis of Several Common APOBEC-type Mutations in Bladder Tumors Suggests Links to Viral Infection.

FGFR3 and PIK3CA are among the most frequently mutated genes in bladder tumors. We hypothesized that recurrent mutations in these genes might be caused by common carcinogenic exposures such as smoking and other factors. We analyzed 2,816 bladder tumors with available data on FGFR3 and/or PIK3CA mutations, focusing on the most recurrent mutations detected in ≥10% of tumors. Compared to tumors with other FGFR3/PIK3CA mutations, FGFR3-Y375C was more common in tumors from smokers than never-smokers (P = 0.009), while several APOBEC-type driver mutations were enriched in never-smokers: FGFR3-S249C (P = 0.013) and PIK3CA-E542K/PIK3CA-E545K (P = 0.009). To explore possible causes of these APOBEC-type mutations, we analyzed RNA sequencing (RNA-seq) data from 798 bladder tumors and detected several viruses, with BK polyomavirus (BKPyV) being the most common. We then performed IHC staining for polyomavirus (PyV) Large T-antigen (LTAg) in an independent set of 211 bladder tumors. Overall, by RNA-seq or IHC-LTAg, we detected PyV in 26 out of 1,010 bladder tumors with significantly higher detection (P = 4.4 × 10-5), 25 of 554 (4.5%) in non-muscle-invasive bladder cancers (NMIBC) versus 1 of 456 (0.2%) of muscle-invasive bladder cancers (MIBC). In the NMIBC subset, the FGFR3/PIK3CA APOBEC-type driver mutations were detected in 94.7% (18/19) of PyV-positive versus 68.3% (259/379) of PyV-negative tumors (P = 0.011). BKPyV tumor positivity in the NMIBC subset with FGFR3- or PIK3CA-mutated tumors was also associated with a higher risk of progression to MIBC (P = 0.019). In conclusion, our results support smoking and BKPyV infection as risk factors contributing to bladder tumorigenesis in the general patient population through distinct molecular mechanisms.

Prevention relevance: Tobacco smoking likely causes one of the most common mutations in bladder tumors (FGFR3-Y375C), while viral infections might contribute to three others (FGFR3-S249C, PIK3CA-E542K, and PIK3CA-E545K). Understanding the causes of these mutations may lead to new prevention and treatment strategies, such as viral screening and vaccination.

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