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家族性非髓样甲状腺癌:临床病理特征、遗传风险因素的当前知识和新进展。

Familial non-medullary thyroid carcinoma: clinico-pathological features, current knowledge and novelty regarding genetic risk factors.

机构信息

Department of Endocrine and Metabolic Diseases, IRCCS Istituto Auxologico Italiano, Milan, Italy -

出版信息

Minerva Endocrinol (Torino). 2021 Mar;46(1):5-20. doi: 10.23736/S2724-6507.20.03338-6. Epub 2020 Oct 12.

DOI:10.23736/S2724-6507.20.03338-6
PMID:33045820
Abstract

Familial non-medullary thyroid cancer (FNMTC) constitutes 3-9% of all thyroid cancers and occurs in two or more first-degree relatives in the absence of predisposing environmental factors. Out of all FNMTC cases, only 5% are represented by syndromic forms (Gardner's Syndrome, familial adenomatous polyposis, Cowden's Syndrome, Carney complex 1, Werner's Syndrome and DICER1 syndrome), in which thyroid cancer occurs as a minor component and the genetic alterations are well-known. The non-syndromic forms represent the majority of all FNMTCs (95%), and the thyroid cancer is the predominant feature. Several low penetration susceptibility risk loci or genes (i.e. TTF1, FOXE1, SRGAP1, SRRM2, HABP2, MAP2K5, and DUOX2), here fully reviewed, have been proposed in recent years with a possible causative role, though the results are still not conclusive or reliable. FNMTC is indistinguishable from sporadic non-medullary thyroid cancer (sNMTC), which means that FNMTC cannot be diagnosed until at least one of the patient's first-degree relatives is affected by tumor. Some studies reported that the non-syndromic FNMTC is more aggressive than the sNMTC, being characterized by a younger age of onset and a higher rate of multifocal and bilateral tumors, extrathyroidal extension, lymph node metastasis, and recurrence. On the contrary, other studies did not find clinical differences between non-syndromic FNMTCs and sporadic cases. Here, I reported an extensive review on genetic and clinico-pathological features of the FNMTC, with particular attention on novel genetic risk factors for non-syndromic forms.

摘要

家族性非髓样甲状腺癌(FNMTC)占所有甲状腺癌的 3-9%,发生于无环境诱发因素的两个或多个一级亲属中。在所有 FNMTC 病例中,只有 5%为综合征形式(Gardner 综合征、家族性腺瘤性息肉病、Cowden 综合征、Carney 综合征 1、Werner 综合征和 DICER1 综合征),其中甲状腺癌作为次要成分出现,遗传改变是已知的。非综合征形式代表了所有 FNMTC 的大多数(95%),并且甲状腺癌是主要特征。近年来,已经提出了几个低外显率易感性风险位点或基因(即 TTF1、FOXE1、SRGAP1、SRRM2、HABP2、MAP2K5 和 DUOX2),尽管结果仍不确定或不可靠,但这些基因可能具有因果作用。FNMTC 与散发性非髓样甲状腺癌(sNMTC)无法区分,这意味着在患者的至少一位一级亲属受到肿瘤影响之前,无法诊断 FNMTC。一些研究报告称,非综合征性 FNMTC 比 sNMTC 更具侵袭性,其特征为发病年龄更轻,多灶性和双侧肿瘤、甲状腺外侵犯、淋巴结转移和复发的发生率更高。相反,其他研究并未发现非综合征性 FNMTC 和散发性病例之间存在临床差异。在这里,我报告了对 FNMTC 的遗传和临床病理特征的广泛综述,特别关注非综合征形式的新遗传危险因素。

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