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Comparison of Genomic Characterization in Upper Tract Urothelial Carcinoma and Urothelial Carcinoma of the Bladder

机译:膀胱上下尿路上皮癌及尿路上皮癌基因组特征的比较

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Background Different genomic characterization in urothelial carcinoma (UC) by site of origin may imply contrasting therapeutic opportunities and pathogenetic mechanisms. The aim of this study was to investigate whether differences between upper tract UC (UTUC) and UC of the bladder (UCB) result from intrinsic biological diversity. Materials and Methods We prospectively sequenced 118 tumors and matched blood DNA from Chinese patients with UC using next-generation sequencing techniques, including 45 UTUC and 73 UCB. Two hundred twenty-six patients with UTUC and 350 patients with UCB for The Cancer Genome Atlas were acquired from the cbioportal. Results There were marked disparities in the mutational landscape for UC according to race and site of origin. Signature 22 for exposure to aristolochic acid was only observed in the UTUC cohort. Conversely, signature 6 for defective DNA mismatch repair only existed in the UCB cohort. Compared with UCB, UTUC had higher clonal and subclonal mutation numbers. TP53 , PIK3CA , and FGFR3 mutations may be the driver genes for UTUC, whereas for UCB, the driver gene may be BRCA1 . Patients with UTUC had lower PD-L1 than those with UCB. There was no significant difference in the number of DDR mutations, copy number variation counts, and tumor mutational burden between UTUC and UCB. Conclusion UTUC and UCB exhibit significant differences in the prevalence of genomic landscape and carcinogenesis. Consequently, molecular subtypes differ according to location, and these results may imply the site-specific management of patients with urothelial carcinoma. Mutational signature may be used as a screening tool to assist clinical differential diagnosis between UTUC and UCB. Implications for Practice This study's findings lay the foundation for a deeper understanding of distinct molecular mechanisms and similar treatment opportunities between upper tract urothelial carcinoma (UTUC) and urothelial carcinoma of the bladder (UCB) and had important implications for the site-specific management of patients with urothelial carcinoma. A comprehensive understanding of the biology of UTUC and UCB is needed to identify new drug targets in order to improve clinical outcomes.
机译:背景技术原产地尿路上皮癌(UC)中的不同基因组特征可能意味着对比治疗机会和致病机理。本研究的目的是探讨膀胱上的上部患者(UTUC)和UC之间的差异是由内在生物多样性产生的。使用下一代测序技术,我们前瞻性地测序118例患有118例患者的血液DNA,使用下一代测序技术,包括45个UTUC和73 UCB。从CBIoportal获得两百二十六名患有UCB的UCB和350名UCB患者。结果根据种族和原产地,UC的突变景观中有明显的差异。仅在Utuc Cohort中观察到暴露于鸟龙酸的签名22。相反,签名6用于缺陷的DNA不匹配修复只存在于UCB队列中。与UCB相比,UTUC具有更高的克隆和亚基突变数。 TP53,PIK3CA和FGFR3突变可以是UTUC的驾驶基因,而对于UCB,驾驶员基因可以是BRCA1。 utuc患者的PD-L1比UCB的患者较低。 DDR突变的数量,拷贝数变异计数和UTUC和UCB之间的肿瘤突变负担没有显着差异。结论utuc和UCB在基因组景观和致癌中的患病率表现出显着差异。因此,分子亚型根据位置而异,这些结果可能意味着尿路上皮癌的患者的特异性特异性管理。突变签名可以用作筛选工具,以帮助utuc和UCB之间的临床鉴别诊断。对实践的影响本研究的研究结果为膀胱(UCB)和膀胱尿路上皮癌(UCB)和尿路上皮癌之间的不同分子机制和类似治疗机会进行了更深的了解,对患者的特异性患者进行了重要意义用尿路上皮癌。需要全面了解utuc和UCB的生物学,以确定新的药物目标,以改善临床结果。

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