Improving diagnostic accuracy of indeterminate thyroid fine needle aspiration using results of ultrasound examination, cyclin D1 immunostaining and molecular testing.

IF 1.6 4区医学 Q3 PATHOLOGY

Acta Cytologica Pub Date : 2025-04-03 DOI:10.1159/000545319

Shurong He, Jingxin Zhang, Mengge Wang, Feiliang Wang, Kan Gao, Rongming Chen, Songtao Hu, Jing Di, Dongge Liu, Mulan Jin

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引用次数: 0

Abstract

Introduction: Fine-needle aspiration (FNA) is the standard procedure for diagnosing thyroid nodules, however indeterminate cytological results present considerable challenges in clinical management. This study aimed to evaluate cyclin D1 immunocytochemistry and Chinese thyroid imaging reporting and data system (C-TIRADS) score, individually and in combination with a simple gene test for cytological diagnosis of Bethesda category Ⅲ‑Ⅴ.

Methods: A consecutive cohort of 177 thyroid FNA specimens with indeterminate diagnoses and available histopathologic follow‑up data were collected. The samples were evaluated by cyclin D1 immunocytochemistry and molecular testing for the BRAFV600E mutation or for a small panel of markers (BRAF, N‑RAS, H‑RAS, K‑RAS and TERT). Two experienced sonographers independently reviewed original sonographic images of each nodule and classified them using the C-TIRADS to reach a consensus score. We evaluated the optimal cut‑off points for cyclin D1 and C-TIRADS scores in diagnosing malignancy using receiver operating characteristic (ROC) curves and the area under the ROC curve (AUC). The specificity, sensitivity, positive predictive value (PPV) and negative predictive value (NPV) of all tests were evaluated with the crosstabs. Logistic regression analysis and ROC curve analysis were used to evaluate the diagnostic accuracy of the three tests individually and combination.

Results: We enrolled 169 patients (177 thyroid nodules), including 140 malignances, 15 low-risk neoplasms, and 22 benign lesions. All 177 specimens were tested for BRAF V600E, while only 21 specimens used the 5-gene detection protocol. With cut-off values set at 10% for cyclin D1 immunocytochemistry and at a C-TIRADS score of 3, along with defining a positive diagnosis as the presence of a mutation in genetic testing, the PPVs for diagnosing thyroid malignancy using the three tests were 97.8%, 90.3%, and 98% respectively; however, the NPVs were 50%, 24.2%, and 26.3 %. The sensitivities were 87.7%, 83.9%, and 63.9%, and the specificities were 86.4%, 36.4% and 90.9%. Regarding AUC, cyclin D1 alone demonstrated greater diagnostic accuracy (0.921, 95%CI=0.857-0.985, P=0.000) compared with the other two methods, which had AUC values of 0.775 (95%CI=0.703-0.846, P=0.000) and 0.587 (95%CI=0.443-0.731, P=0.235). The combination of two or three tests yielded higher accuracy (0.929, 95%CI=0.873-0.985, P=0.000; 0.925, 95%CI=0.860-0.989, P=0.000; 0.937, 95%CI=0.889-0.985, P=0.000) compared with cyclin D1 immunocytochemistry alone (0.921, 95%CI=0.857-0.985, P=0.000).

Conclusion: Adding cyclin D1 immunocytochemistry or a simple gene panel test, alone or in combination, significantly enhances the diagnostic value of the C-TIRADS score in thyroid nodules with indeterminate cytology. Laboratories should integrate these tests to effectively manage uncertain thyroid nodules and reduce diagnostic ambiguity.

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超声检查、细胞周期蛋白D1免疫染色及分子检测提高甲状腺细针穿刺不确定的诊断准确性。

细针穿刺（FNA）是诊断甲状腺结节的标准方法，然而不确定的细胞学结果给临床管理带来了相当大的挑战。本研究旨在评估细胞周期蛋白D1免疫细胞化学和中国甲状腺成像报告和数据系统（C-TIRADS）评分，单独或结合简单的基因检测用于Bethesda分类Ⅲ‑Ⅴ的细胞学诊断。方法：收集177例诊断不明确的甲状腺FNA标本和可用的组织病理学随访资料。通过细胞周期蛋白D1免疫细胞化学和分子检测对样本进行BRAFV600E突变或一小组标记（BRAF、N - RAS、H - RAS、K - RAS和TERT）的评估。两名经验丰富的超声医师独立审查了每个结节的原始超声图像，并使用C-TIRADS对其进行分类，以达成共识评分。我们使用受试者工作特征（ROC）曲线和ROC曲线下面积（AUC）评估cyclin D1和C-TIRADS评分诊断恶性肿瘤的最佳截断点。采用交叉表法评价各指标的特异性、敏感性、阳性预测值（PPV）和阴性预测值（NPV）。采用Logistic回归分析和ROC曲线分析评价三项检测单独及联合诊断的准确性。结果：我们纳入169例患者（177例甲状腺结节），包括140例恶性肿瘤，15例低危肿瘤和22例良性病变。所有177份标本均检测BRAF V600E，仅有21份标本采用5基因检测方案。周期蛋白D1免疫细胞化学的临界值为10%，C-TIRADS评分为3分，并将阳性诊断定义为基因检测中存在突变，使用这三种检测诊断甲状腺恶性肿瘤的ppv分别为97.8%、90.3%和98%；npv分别为50%、24.2%和26.3%。敏感性分别为87.7%、83.9%、63.9%，特异性分别为86.4%、36.4%、90.9%。在AUC方面，单独使用cyclin D1的诊断准确率（0.921,95%CI=0.857 ~ 0.985， P=0.000）高于其他两种方法的AUC值分别为0.775 （95%CI=0.703 ~ 0.846， P=0.000）和0.587 （95%CI=0.443 ~ 0.731， P=0.235）。2次或3次联合检测准确率较高(0.929,95%CI=0.873 ~ 0.985， P=0.000；0.925, 95%ci =0.860-0.989, p =0.000；0.937, 95%CI=0.889-0.985， P=0.000)，与单纯cyclin D1免疫细胞化学比较（0.921,95%CI=0.857-0.985， P=0.000）。结论：单独或联合应用cyclin D1免疫细胞化学或简单的基因面板检测，可显著提高C-TIRADS评分对细胞学不确定的甲状腺结节的诊断价值。实验室应整合这些测试，以有效地管理不确定的甲状腺结节，减少诊断的模糊性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Acta Cytologica 生物-病理学

CiteScore

3.70

自引率

11.10%

发文量

审稿时长

4-8 weeks

期刊介绍： With articles offering an excellent balance between clinical cytology and cytopathology, ''Acta Cytologica'' fosters the understanding of the pathogenetic mechanisms behind cytomorphology and thus facilitates the translation of frontline research into clinical practice. As the official journal of the International Academy of Cytology and affiliated to over 50 national cytology societies around the world, ''Acta Cytologica'' evaluates new and existing diagnostic applications of scientific advances as well as their clinical correlations. Original papers, review articles, meta-analyses, novel insights from clinical practice, and letters to the editor cover topics from diagnostic cytopathology, gynecologic and non-gynecologic cytopathology to fine needle aspiration, molecular techniques and their diagnostic applications. As the perfect reference for practical use, ''Acta Cytologica'' addresses a multidisciplinary audience practicing clinical cytopathology, cell biology, oncology, interventional radiology, otorhinolaryngology, gastroenterology, urology, pulmonology and preventive medicine.