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膀胱肿瘤基底鳞状亚型中分子亚型分类不一致及其配对淋巴结转移。

Discordant molecular subtype classification in the basal-squamous subtype of bladder tumors and matched lymph-node metastases.

机构信息

Division of Urological Research, Department of Translational Medicine, Lund University, Lund, Sweden.

Department of Urology, Skåne University Hospital, Malmö, Sweden.

出版信息

Mod Pathol. 2018 Dec;31(12):1869-1881. doi: 10.1038/s41379-018-0096-5. Epub 2018 Jul 2.

Abstract

Molecular subtypes of muscle-invasive bladder tumors have emerged as a promising research tool with potential to stratify patients for neoadjuvant treatment. Prior to radical cystectomy, the utility of molecular classification and biomarkers depend on concordance between tissue from transurethrally resected specimens and disseminated disease. We assess the concordance of molecular subtypes and a large number of potential biomarkers in 67 pairs of muscle-invasive bladder tumors and synchronous lymph-node metastases. Tissue cores were stained for 29 immunohistochemistry markers and immunohistochemistry-based molecular subtype classification was performed. Molecular subtype was determined by mRNA profiling for 57 bladder tumors and 28 matched lymph-node metastases. Full section immunohistochemistry was performed to assess intra-tumor subtype heterogeneity in discordant cases, and exome sequencing was performed for 20 sample pairs. Discordant subtype classification between the bladder tumor and lymph-node metastasis was generally rare (12/67, 18%), but most (7/12, 58%) involved the Basal/Squamous-like subtype. Discordant Basal/Squamous-like tumors showed either Urothelial-like or Genomically Unstable, luminal-like phenotype in the lymph-node metastasis. Full section immunohistochemistry revealed intra-tumor subtype heterogeneity for six discordant cases including four involving the Basal/Squamous-like subtype. Subtype concordance for non- Basal/Squamous-like tumors was 91%. RNA-based classification agreed with immunohistochemistry classification but quantitative assessment is necessary to avoid false detection of subtype shifts. Most high confidence cancer mutations were shared between samples (n = 93, 78%), and bladder tumor private mutations (n = 20, 17%) were more frequent than those private to the lymph-node metastasis (n = 7, 6%). We conclude that bladder tumors and lymph-node metastases have overall similar molecular subtype, biomarker expression, and cancer mutations. The main exception was tumors of the Basal/Squamous-like subtype where most cases showed discordant classification, some with evidence of intra-tumor heterogeneity. The data are of relevance for neoadjuvant treatment stratification and raises questions on the dynamics of molecular subtypes during bladder cancer progression.

摘要

肌层浸润性膀胱癌的分子亚型已成为一种很有前途的研究工具,具有对新辅助治疗进行分层的潜力。在根治性膀胱切除术之前,分子分类和生物标志物的效用取决于经尿道切除标本和播散性疾病之间的一致性。我们评估了 67 对肌层浸润性膀胱癌和同步淋巴结转移瘤中大量潜在生物标志物的分子亚型的一致性。对组织芯进行了 29 种免疫组织化学标志物染色,并进行了基于免疫组织化学的分子亚型分类。对 57 例膀胱癌和 28 例匹配的淋巴结转移瘤进行了 mRNA 分析以确定分子亚型。对 20 对样本进行了全切片免疫组织化学以评估不一致病例的肿瘤内亚型异质性,并进行了外显子测序。膀胱癌和淋巴结转移瘤之间的亚型分类通常很少见(12/67,18%),但大多数(7/12,58%)涉及基底/鳞状样亚型。在淋巴结转移中,不一致的基底/鳞状样肿瘤表现为尿路上皮样或基因组不稳定的亮细胞样表型。全切片免疫组织化学显示,6 例不一致病例中有 4 例涉及基底/鳞状样亚型存在肿瘤内亚型异质性。非基底/鳞状样肿瘤的亚型一致性为 91%。基于 RNA 的分类与免疫组织化学分类一致,但需要进行定量评估以避免亚型转换的假检测。大多数高可信度的癌症突变在样本之间共享(n=93,78%),而膀胱癌特有的突变(n=20,17%)比淋巴结转移特有的突变(n=7,6%)更频繁。我们的结论是,膀胱癌和淋巴结转移瘤具有总体相似的分子亚型、生物标志物表达和癌症突变。主要的例外是基底/鳞状样亚型的肿瘤,其中大多数病例表现出不一致的分类,一些病例有肿瘤内异质性的证据。这些数据与新辅助治疗分层有关,并提出了关于膀胱癌进展过程中分子亚型动态的问题。

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