Department of Endocrine and Metabolic Diseases, Istituto di Ricovero e Cura a Carattere Scientifico (IRCCS) Istituto Auxologico Italiano, Milan, Italy.
Department of Pathophysiology and Transplantation, Università degli Studi di Milano, Milan, Italy.
Front Endocrinol (Lausanne). 2021 Jan 7;11:589340. doi: 10.3389/fendo.2020.589340. eCollection 2020.
Several low penetration susceptibility risk loci or genes have been proposed in recent years with a possible causative role for familial non-medullary thyroid cancer (FNMTC), though the results are still not conclusive or reliable. Among all the candidates, here fully reviewed, a new extremely rare germline variant c.3607A>G (p.Y1203H) of the gene, has been recently reported to co-segregate with the affected members of one non-syndromic FNMTC family. We aimed to validate this finding in our series of 33 unrelated FNMTC Italian families, previously found to be negative for two susceptibility germline variants in the and genes. Unfortunately, the p.Y1203H variant was not found in either the 74 affected or the 12 not affected family members of our series. We obtained interesting data by comparing the clinico-pathological data of the affected members of our kindreds with a large consecutive series of sporadic cases, followed at our site. We found that familial tumors had a statistically significant more aggressive presentation at diagnosis, though not resulting in a worst outcome. In conclusion, we report genetic and clinical data in a large series of FNMTC kindreds. Our families are negative for variants reported as likely causative, namely those lying in the , and genes. The extensive review of the current knowledge on the genetic risk factors for non-syndromic FNMTCs underlies how the management of these tumors remains mainly clinical. Despite the more aggressive presentation of familial cases, an appropriate treatment leads to an outcome similar to that observed for sporadic cases.
近年来,已经提出了几个低穿透性易感性风险位点或基因,这些基因可能与家族性非髓样甲状腺癌(FNMTC)有关,但结果仍不确定或不可靠。在所有的候选基因中,我们对 基因的一个新的极其罕见的种系变异 c.3607A>G(p.Y1203H)进行了全面的回顾,该变异最近被报道与一个非综合征性 FNMTC 家族的受影响成员共分离。我们旨在验证这一发现,为此,我们对 33 个无关的意大利 FNMTC 家族进行了研究,这些家族先前被发现两个易感性种系变异在 和 基因中均为阴性。不幸的是,在我们的研究中,74 名受影响的和 12 名未受影响的家族成员均未发现 基因 p.Y1203H 变异。通过比较我们家系中受影响成员的临床病理数据与我们单位随访的大量连续散发性病例的临床病理数据,我们获得了有趣的数据。我们发现,家族性肿瘤在诊断时的表现更为侵袭性,但并不导致预后更差。总之,我们报道了一个大型 FNMTC 家系的遗传和临床数据。我们的家族中没有报道为可能的致病原因的变异,即那些位于 、 和 基因中的变异。对非综合征性 FNMTC 的遗传风险因素的现有知识的广泛回顾,说明了这些肿瘤的管理主要仍然是临床的。尽管家族性病例的表现更为侵袭性,但适当的治疗可导致与散发性病例相似的结果。
