通过分子衍生的恶性肿瘤风险和其他相关参数解析甲状腺细胞病理学中的恶性肿瘤诊断可疑病例:洞察结节特征和实践模式

IF 2.6 3区 医学 Q3 ONCOLOGY Cancer Cytopathology Pub Date : 2024-09-11 DOI:10.1002/cncy.22904
David Starr, Youley Tjendra, Jaylou M. Velez Torres, Carmen Gomez‐Fernandez, Samer N. Khader, Esra Karslioglu‐French, Linwah Yip, Sally E. Carty, John M. Skaugen, Yuri E. Nikiforov, Raja R. Seethala, N. Paul Ohori
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引用次数: 0

摘要

导言:甲状腺细胞病理学病例被诊断为可疑恶性肿瘤(SFM)后,通常会进行切除手术。然而,分子检测提供的细节可能会带来更多的启示。本研究对两家常规使用ThyroSeq v3(TSV3)的机构的SFM病例的分子图谱进行了研究。材料与方法经机构审查委员会批准后,从两家机构的数据库中检索了有TSV3结果的SFM甲状腺细胞病理学病例。计算包括恶性肿瘤分子衍生风险(MDROM)在内的分子信息、细胞学与组织学相关数据以及其他相关参数。结果核心数据集包括 114 个通过 TSV3 质量保证的 SFM 病例。所有 TSV3 结果均报告为基因组改变的阳性或阴性,除 5 例病例外,其他病例均提供了恶性肿瘤的概率估计。总体合并基线 MDROM 为 75.7%(95% CI,70.0-81.4),与 Bethesda 系统公布的恶性肿瘤风险(74%)相当。切除组和未切除组的合并 MDROMs 有显著统计学差异(79.0% vs 58.6%; p = .0153)。有趣的是,两家机构切除组的 MDROMs 也有统计学差异(75.0% vs 85.3%; p = .020)。细胞学-组织学相关性显示,88.5%的切除病例有恶性结果。结论 对SFM病例的分子分析表明,高风险基因组改变与组织学上明显的肿瘤相关,导致恶性结果较基线增加。MDROM分析表明,两家机构对滤泡型肿瘤的细胞病理学实践模式存在差异。
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Parsing the thyroid cytopathology suspicious for malignancy diagnosis through molecular‐derived risk of malignancy and other related parameters: Insights into nodule characteristics and practice patterns
IntroductionThyroid cytopathology cases with suspicious for malignancy (SFM) diagnosis often result in resection. However, molecular testing offers details that may provide additional insights. In this study, the molecular profiles of SFM cases from two institutions that routinely used ThyroSeq v3 (TSV3) were examined.Materials and MethodsFollowing institutional review board approval, SFM thyroid cytopathology cases with TSV3 results were retrieved from the databases of two institutions. Molecular information including molecular‐derived risk of malignancy (MDROM), cytologic‐histologic correlation data, and other related parameters were calculated. Statistical comparisons were made with a p <.05 considered significant.ResultsThe core data set comprised 114 SFM cases that passed TSV3 quality assurance. All TSV3 results were reported as positive or negative for genomic alterations and all except five cases provided a probability of malignancy estimate. The overall combined baseline MDROM of 75.7% (95% CI, 70.0–81.4) was comparable to the risk of malignancy (74%) published in the Bethesda System. There was a statistically significant difference between the combined MDROMs of resected and unresected cohorts (79.0% vs 58.6%; p = .0153). Interestingly, the MDROMs of the resected cohorts from the two institutions were statistically different (75.0% vs 85.3%; p = .020). Cytologic–histologic correlation revealed malignant outcome in 88.5% of resected cases.ConclusionsMolecular analyses of SFM cases demonstrated higher risk genomic alterations that were associated with histologically overt neoplasms, resulting in increased malignancy outcome compared to baseline. MDROM analysis revealed differences in the cytopathologic practice patterns regarding follicular‐patterned neoplasms at the two institutions.
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来源期刊
Cancer Cytopathology
Cancer Cytopathology 医学-病理学
CiteScore
7.00
自引率
17.60%
发文量
130
审稿时长
1 months
期刊介绍: Cancer Cytopathology provides a unique forum for interaction and dissemination of original research and educational information relevant to the practice of cytopathology and its related oncologic disciplines. The journal strives to have a positive effect on cancer prevention, early detection, diagnosis, and cure by the publication of high-quality content. The mission of Cancer Cytopathology is to present and inform readers of new applications, technological advances, cutting-edge research, novel applications of molecular techniques, and relevant review articles related to cytopathology.
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