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β-连环蛋白、Pax2 和 Pten 联合检测可识别组织学亚诊断性子宫内膜病变中的癌前病变。

β-catenin, Pax2, and Pten Panel Identifies Precancers Among Histologically Subdiagnostic Endometrial Lesions.

机构信息

Departments of Pathology.

Obstetrics and Gynecology.

出版信息

Am J Surg Pathol. 2023 May 1;47(5):618-629. doi: 10.1097/PAS.0000000000002034. Epub 2023 Mar 20.

DOI:10.1097/PAS.0000000000002034
PMID:36939046
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10101134/
Abstract

Despite refinements in histologic criteria for the diagnosis of endometrioid precancers, many challenging cases are encountered in daily practice, creating diagnostic uncertainty and suboptimal patient management. Recently, an immunohistochemical 3-marker panel consisting of β-catenin, Pax2, and Pten was identified as a useful diagnostic adjunct. However, previous studies focused either on cancers or diagnostically unambiguous precancers, leaving questions about the applicability and utility of the panel in endometria with architectural features near or below the threshold of accepted histologic criteria for endometrioid precancers. Here, in a retrospective study of 90 patients, we evaluated the performance of the 3-marker panel. Notably, the panel detected a subset of disordered proliferative endometria (8/44, 18%), nonatypical hyperplasias (19/40, 48%), and cases with ambiguous features (3/6, 50%) with aberrancy for ≥1 markers. Marker-aberrant cases were more likely to progress to endometrioid precancer or cancer ( P =0.0002). Patterns of marker aberrancy in the index and progressor cases from individual patients provided evidence for origin in a common precursor, and next-generation sequencing of the progressor cases rationalized marker aberrancy for β-catenin and Pten. The results unequivocally demonstrate that some lesions that do not approach current histologic thresholds are bona fide neoplastic precursors with clinically-relevant driver events that can be detected by the 3-marker panel. The findings provide further validation for the diagnostic utility of the panel in clinical practice and its application in difficult or ambiguous cases.

摘要

尽管在子宫内膜样癌前病变的组织学诊断标准方面已经有所改进,但在日常实践中仍会遇到许多具有挑战性的病例,导致诊断不确定和患者管理不理想。最近,一种由β-连环蛋白、Pax2 和 Pten 组成的免疫组织化学 3 标志物面板被确定为一种有用的诊断辅助手段。然而,之前的研究要么集中在癌症上,要么集中在诊断明确的癌前病变上,因此关于该面板在接近或低于子宫内膜样癌前病变公认组织学标准的结构特征的子宫内膜中的适用性和实用性仍存在疑问。在这里,我们在一项对 90 例患者的回顾性研究中评估了该 3 标志物面板的性能。值得注意的是,该面板检测到紊乱性增生性子宫内膜(8/44,18%)、非典型增生(19/40,48%)和具有模糊特征的病例(3/6,50%)的一组病例,其≥1 个标志物出现异常。标志物异常病例更有可能进展为子宫内膜样癌前病变或癌症(P=0.0002)。来自单个患者的索引和进展病例的标志物异常模式为共同前体起源提供了证据,并且对进展病例的下一代测序合理地解释了β-连环蛋白和 Pten 的标志物异常。这些结果明确表明,一些未达到当前组织学阈值的病变是真正的肿瘤前体,具有临床相关的驱动事件,可通过 3 标志物面板检测到。这些发现进一步验证了该面板在临床实践中的诊断实用性及其在困难或模糊病例中的应用。

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