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循环肿瘤DNA检测在早期高分化甲状腺癌患者中的临床及诊断效用有限:与良性甲状腺结节及健康个体的比较

Limited Clinical and Diagnostic Utility of Circulating Tumor DNA Detection in Patients with Early-Stage Well-Differentiated Thyroid Cancer: Comparison with Benign Thyroid Nodules and Healthy Individuals.

作者信息

Suh Yong Joon, Kwon Mi Jung, Noh Hye-Mi, Lee Hong Kyu, Ra Yong Joon, Kim Nan Young

机构信息

Department of Breast and Endocrine Surgery, Hallym University Sacred Heart Hospital, Hallym University College of Medicine, 22, Gwanpyeong-ro 170 beon-gil, Dongan-gu, Anyang-si 14068, Gyeonggi-do, Korea.

Department of Pathology, Hallym University Sacred Heart Hospital, Hallym University College of Medicine, 22, Gwanpyeong-ro 170 beon-gil, Dongan-gu, Anyang-si 14068, Gyeonggi-do, Korea.

出版信息

Healthcare (Basel). 2021 Apr 1;9(4):386. doi: 10.3390/healthcare9040386.

Abstract

Limited data are available on the diagnostic utility of circulating tumor DNA (ctDNA) in early-stage thyroid cancers for , , , and promoter mutations, which are known detectable markers for thyroid cancers. Here, we analyzed the above driver mutations in ctDNA and matched neoplastic tissues from patients with early-stage thyroid cancers in order to investigate diagnostic utility of circulating markers in distinguishing from other mimicking thyroid lesions and healthy individuals. In total, 73 matched neoplastic tissue and plasma samples [thyroid cancers (n = 62), benign thyroid disorders (n = 8), and parathyroid lesions (n = 3)] and 54 plasma samples from healthy individuals (as controls) were analyzed for , , , and promoter mutations using peptide nucleic acid clamp real-time PCR. Although only one patient with an indeterminate lesion on thyroid cytology showed mutation (codon 146) in the preoperative plasma, that mutation was not identified in the stage I papillary thyroid carcinoma tissue. In the remaining 72 plasma samples, no other mutations were identified in , , and promoter genes. The concordance rates of mutational results between the plasma and tumor tissue or metastatic lymph node were very low. One (1.9%) of the 54 healthy individuals harbored a mutation in the plasma samples. The ctDNA results did not represent the mutational profile of primary or metastatic thyroid cancers, warranting a caution for interpretation. The clinical utility of , , , and promoter mutation analysis on ctDNA appears to be limited to early-stage thyroid cancers.

摘要

关于循环肿瘤DNA(ctDNA)在早期甲状腺癌中对于 、 、 和 启动子突变的诊断效用的可用数据有限,这些突变是已知的甲状腺癌可检测标志物。在此,我们分析了早期甲状腺癌患者ctDNA和匹配的肿瘤组织中的上述驱动突变,以研究循环标志物在区分其他类似甲状腺病变和健康个体方面的诊断效用。总共对73对匹配的肿瘤组织和血浆样本[甲状腺癌(n = 62)、良性甲状腺疾病(n = 8)和甲状旁腺病变(n = 3)]以及54份来自健康个体的血浆样本(作为对照)使用肽核酸钳实时PCR分析了 、 、 和 启动子突变。虽然只有一名甲状腺细胞学检查结果不确定的患者在术前血浆中显示 突变(密码子146),但在I期乳头状甲状腺癌组织中未发现该 突变。在其余72份血浆样本中,在 、 和 启动子基因中未发现其他突变。血浆与肿瘤组织或转移淋巴结之间突变结果的一致率非常低。54名健康个体中有1名(1.9%)在血浆样本中携带 突变。ctDNA结果并不代表原发性或转移性甲状腺癌的突变谱,在解释时需谨慎。对ctDNA进行 、 、 和 启动子突变分析的临床效用似乎仅限于早期甲状腺癌。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d003/8065614/777109dc3901/healthcare-09-00386-g001.jpg

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