Urachal and Nonurachal Adenocarcinomas of the Urinary Bladder: A Comprehensive Genomic Profiling Study.

IF 5.3 2区 医学 Q1 ONCOLOGY JCO precision oncology Pub Date : 2024-08-01 DOI:10.1200/PO.24.00200
Antonio Cigliola, Alina Basnet, Joseph M Jacob, Chiara Mercinelli, Valentina Tateo, Damiano Alfio Patanè, Gennady Bratslavsky, Liang Cheng, Petros Grivas, Ashish M Kamat, Philippe E Spiess, Dean C Pavlick, Douglas I Lin, Jeffrey S Ross, Andrea Necchi
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Abstract

Purpose: Although both urachal (U) and nonurachal (NU) bladder adenocarcinomas (adenoCas) share several histologic similarities, they differ in location and sometimes in therapeutic options. We analyzed the differences in genomic alterations (GAs) between these tumor entities, with the aim of identifying potential therapeutic targets for clinical trials.

Materials and methods: Overall, 133 U and 328 NU adenoCas were analyzed. Hybrid capture-based comprehensive genomic profiling (CGP) was performed to evaluate all classes of GA. Germline status of GA was predicted using a validated somatic-germline computational method. CGP was performed using the FoundationOne and FoundationOne CDx assays (Foundation Medicine, Inc).

Results: The most frequent GA in both U and NU cohorts included TP53 (86.5% v 81.1%) and KRAS (34.6% v 27.7%). GAs characteristic of colorectal adenoCa, such as SMAD4 (P = .069) and GNAS (P = .071), were more common in U versus NU. Conversely, TERT (P < .01) and RB1 (P = .071) were more prevalent in NU adenoCa. Notably, both U and NU adenoCas exhibited possibly targetable GA in PIK3CA (7.5% v 7.9%) and ERBB2 (6.8% v 7.6%). Biomarkers associated with potential benefit from anti-PD-1/L1 were infrequent. Median tumor mutational burden was 2.6 and 3.5 mutations per megabase for U and NU, respectively, and PD-L1 expression >1% was rare. Genomic ancestry and genomic signature distribution were similar in both tumor types. GAs were most commonly of somatic nature. Limitations include lack of clinical data, tumor heterogeneity, and retrospective nature.

Conclusion: U and NU adenoCAs revealed differences in GA, with PIK3CA and ERBB2 being identified as putative therapeutic targets. Biomarkers of response to anti-PD-(L)1 were uncommon. Results highlight the potential of CGP to personalize treatment options of bladder adenoCa and inform clinical trial designs.

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膀胱尿道腺癌和非尿道腺癌:综合基因组剖析研究
目的:虽然尿道(U)膀胱腺癌(adenoCas)和非尿道(NU)膀胱腺癌(adenoCas)在组织学上有一些相似之处,但它们的位置不同,有时治疗方案也不同。我们分析了这些肿瘤实体之间基因组改变(GAs)的差异,目的是为临床试验确定潜在的治疗靶点:总共分析了 133 例 U 型腺癌和 328 例 NU 型腺癌。进行了基于混合捕获的综合基因组图谱分析(CGP),以评估所有类别的GA。使用经过验证的体细胞-种系计算方法预测 GA 的种系状态。CGP使用FoundationOne和FoundationOne CDx测定(Foundation Medicine, Inc)进行:结果:在 U 和 NU 队列中,最常见的 GA 包括 TP53(86.5% 对 81.1%)和 KRAS(34.6% 对 27.7%)。具有结直肠腺癌特征的GA,如SMAD4(P = .069)和GNAS(P = .071),在U组和NU组中更为常见。相反,TERT(P < .01)和 RB1(P = .071)在 NU 腺癌中更为常见。值得注意的是,U腺癌和NU腺癌中的PIK3CA(7.5% v 7.9%)和ERBB2(6.8% v 7.6%)都表现出可能的靶向性GA。与抗 PD-1/L1 潜在获益相关的生物标志物并不常见。U和NU的中位肿瘤突变负荷分别为2.6和3.5个突变/兆碱基,PD-L1表达>1%的情况很少见。两种肿瘤类型的基因组祖先和基因组特征分布相似。体细胞基因组特征最常见。不足之处包括缺乏临床数据、肿瘤异质性和回顾性:结论:U腺癌和NU腺癌显示出GA的差异,PIK3CA和ERBB2被确定为潜在的治疗靶点。对抗PD-(L)1反应的生物标志物并不常见。研究结果凸显了CGP在个性化膀胱腺癌治疗方案和临床试验设计方面的潜力。
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CiteScore
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