左侧异位甲状腺癌变误诊为甲状舌管囊肿一例

患者，男，53岁，因发现“颈前肿物2个月，近1周迅速增大”而入院。查体：颈前正中舌骨下方可触及大小约1．7cm×0．8cm×1．1cm肿物，边界清楚，表面光滑，质地软，无触痛及压痛，无震颤，可随伸缩舌而上下活动。颈部彩色超声提示：甲状腺大小形态正常，左叶腺体回声稍减低，分布欠均匀；彩色多普勒（CDFI）：血流信号未见增加，可见星点状血流信号；肿物CT扫描：可见一实质性肿物，大小约16mm×9mm×11mm，边界清楚，呈近低回声，形态欠规则，内部回声不均，可见多个细点状钙化回声，颈部未见淋巴结肿大。

14例结节性甲状腺肿并发癌变的诊治体会

目的 总结 14例结节性甲状腺肿并发癌变的诊断和外科治疗经验。方法 回顾分析 14例结节性甲状腺肿并发癌变的临床资料。结果 14例均于术前明确诊断为结节性甲状腺肿 ,都未取得癌变的确诊依据。再次治疗的方法选择不同。结论 在诊断为结节性甲状腺肿 ,而存在并发癌变可能的患者治疗中 ,手术方式的选择很重要。

桥本氏病患者血清甲状腺激素水平与甲状腺组织癌变的相关性

目的探讨桥本氏病患者血清甲状腺激素(TSH)水平与甲状腺组织癌变的相关性。方法回顾性分析2016年6月至2019年6月医院收治的102例桥本氏病患者的临床资料,根据有无出现甲状腺组织癌变分为A组(有甲状腺组织癌变)和B组(无甲状腺组织癌变),各51例,比较两组血清TSH水平,并分析TSH和甲状腺组织癌变的相关性。结果 B组血清TSH水平低于A组,差异有统计学意义(P<0.05);经Pearson分析,桥本氏病患者血清TSH水平与甲状腺组织癌变成正相关(P<0.05)。结论桥本氏病患者出现甲状腺组织癌变将造成血清TSH水平升高,且血清TSH水平升高会增加甲状腺组织发生癌变的风险。

桥本氏病合并甲状腺乳头状癌患者血清甲状腺相关激素水平的变化及意义

目的:探究桥本氏病(HT)合并甲状腺乳头状癌(PTC)患者血清甲状腺相关激素水平的变化及意义。方法:对我院148例HT患者的临床资料进行回顾性分析,根据其是否合并PTC分为HT合并PTC组(n=68)和单纯HT组(n=80)。比较两组患者性别、年龄及血清促甲状腺激素(TSH)、甲状腺功能指标[游离三碘甲腺原氨酸(FT3)、游离甲状腺素(FT4)]、抗甲状腺抗体[甲状腺球蛋白抗体(TGAb)、甲状腺过氧物酶抗体(TPOAb)]水平等临床资料差异,分析血清TSH水平变化及意义。结果:HT合并PTC组患者男性比例、年龄、病程及血清TSH水平均大于单纯HT组,血清TGAb、TPOAb水平则均小于单纯HT组(P<0.05);血清FT3、FT4水平比较差异无统计学意义(P>0.05)。HT合并PTC患者组血清TSH>4.2 m IU/L患者占比高于血清TSH正常组(P<0.05)。血清TSH>4.2 m IU/L患者中HT合并PTC患者的占比大于血清TSH水平正常的患者(P<0.05)。HT合并PTC患者中,血清TSH水平>4.2 m IU/L患者中央区淋巴结转移发生率高于血清TSH水平正常患者(P<0.05);血清TSH>4.2 m IU/L与血清TSH正常患者多灶癌发生率比较差异无统计学意义(P>0.05)。结论:HT患者血清TSH水平升高可能促进其甲状腺组织癌变,HT合并PTC患者血清TSH水平升高可能促进其中央区淋巴结转移。

Correlation between BRAF^(V600E) mutation and clinicopathological features in pediatric papillary thyroid carcinoma

In adults, the presence of the BRAF^(V600E) mutation in papillary thyroid cancer(PTC) has been demonstrated to be strongly associated with aggressive cancer-cell characteristics and poor patient prognosis. In contrast, the frequency of this mutation in pediatric PTC has undergone limited study, and the few available estimates range from 0 to 63%. Furthermore, the role of the BRAF^(V600E) mutation in pediatric PTC is controversial; thus, the present study aimed to investigate the prevalence and role of the BRAF^(V600E) mutation in48 pediatric patients with PTC, aged 3–13 years. Of these patients, 41 were diagnosed with classic PTC, five were found to have a follicular variant of PTC, and two to exhibit a diffuse sclerosing PTC variant. The BRAF^(V600E) mutation was identified to be present in 35.4% of the 48 analyzed patients, and in 41.5% of the patients diagnosed with classical PTC. Furthermore, the presence of the BRAF^(V600E) mutation was found to be associated with a patient age at diagnosis of less than ten years(P=0.011), the performance of a thyroidectomy(P=0.03), exhibited tumor multifocality(P=0.02) and/or extra-thyroidal invasion(P=0.003), and both a low MACIS(Metastases, Age, Completeness of resection, Invasion, Size)(P=0.036) and AMES(Age, Metastasis, Extent of tumor,Size)(P=0.001)score. Together, these data suggest that the presence of the BRAF^(V600E) mutation may be negatively correlated with partial aggressive clinicopathological features of pediatric PTC.