甲状腺滤泡癌的诊断问题

S. Titov, S. A. Lukyanov, S. V. Sergiyko, Y. Veryaskina, T. E. Ilyina, E. S. Kozorezov, S. Vorobyov
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摘要

导言滤泡状甲状腺癌比乳头状甲状腺癌少见得多。然而,术前诊断的主要困难与这种形态类型有关。细针穿刺活检无法区分良性滤泡腺瘤和滤泡癌,这迫使外科医生对所有细胞学结论为 "滤泡性肿瘤 "的患者进行甲状腺诊断性切除。通过新一代测序寻找滤泡癌特异性微RNA。分析了 2021 年至 2022 年在车里雅宾斯克内分泌外科中心手术的术前细胞学结论为 "滤泡肿瘤 "的患者数据。病理学家对组织学制剂进行了两次审查。对 8 份滤泡癌组织学样本和 8 份滤泡腺瘤样本进行了基因组测序。所选 microRNAs 的表达水平与 198 份归档的各类甲状腺肿瘤细胞学样本进行了比较。细胞学结论为 "滤泡瘤 "的恶性肿瘤风险为 25.4%(误差为 74.6%)。首次发现滤泡癌的患者有 36 人,发病率为每年每 10 万人新增病例 0.68 例。有 8 例(36.4%)患者的 "滤泡癌 "诊断得到了 3 位形态学专家的确认。测序结果显示,滤泡癌和滤泡腺瘤之间存在 5 种最不同的 microRNA:miR-625、miR-323a、let-7a、let-7c 和 miR-574。利用我们选择的 microRNAs 区分卵泡腺瘤和卵泡癌的误差率为 21%(交叉验证为 35%)。与细胞学研究相比,术前阶段旨在区分滤泡癌和滤泡腺瘤的分子遗传学研究具有更高的准确性,但不足以做出最终的临床决定。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Problems of follicular thyroid carcinoma diagnostics
Introduction. Follicular thyroid cancer is much less common than papillary cancer. Nevertheless, the main difficulties in preoperative diagnosis are associated with this morphological type. A fine needle aspiration biopsy is not able to distinguish a benign follicular adenoma from a follicular carcinoma, which forces surgeons to perform diagnostic resection of the thyroid gland in all patients with a cytological conclusion «follicular tumor».Aim. To search for microRNAs specific to follicular cancer by sequencing a new generation.Materials and methods. The data of patients with a preoperative cytological conclusion «follicular tumor» operated at the Chelyabinsk Center for Endocrine Surgery from 2021 to 2022 were analyzed. Histological preparations were reviewed twice by pathologists. Genome sequencing was performed in 8 histological samples of follicular cancer and 8 samples of follicular adenoma. The expression levels of the selected microRNAs were compared with 198 archived cytological samples of various types of thyroid tumors.Results. The risk of malignancy at the cytological conclusion «follicular tumor» was 25.4 % (error 74.6 %). Follicular cancer was first detected in 36 patients, the incidence was 0.68 new cases per 100 thousand population per year. The diagnosis of «follicular cancer» was confirmed by 3 morphologists in 8 (36.4 %) cases. Sequencing revealed the 5 most distinct microRNAs between follicular cancer and follicular adenoma: miR-625, miR-323a, let-7a, let-7c and miR-574. The level of errors in the differentiation of follicular adenoma and follicular cancer using the microRNAs we selected was 21 % (35 % with cross-validation).Conclusion. Molecular genetic research at the preoperative stage, aimed at differentiating follicular cancer and follicular adenoma, in comparison with cytological research has a greater, but insufficient accuracy for making a final clinical decision.
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