单中心回顾性系列黑色素瘤患者中 CDKN2A、CDK4、POT1、BAP1、MITF、ATM 和 TERT 致病性变异的患病率以及提示遗传倾向的个人或家族史。

IF 2.5 4区 医学 Q2 DERMATOLOGY
Giada Ferrara, Salvatore Paiella, Giulio Settanni, Melissa Frizziero, Paolo Rosina, Valeria Viassolo
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引用次数: 0

摘要

简介:约 20%-45% 的家族性黑色素瘤(FM)病例与遗传易感性有关:大约20%-45%的家族性黑色素瘤(FM)病例与遗传易感性有关:这项单中心回顾性研究旨在评估皮肤黑色素瘤患者主要黑色素瘤易感基因中致病变体(PV)的频率,并调查遗传易感性的临床预测因素:方法:纳入的患者为2000年至2022年期间在意大利维罗纳大学医院皮肤科确诊的皮肤黑色素瘤患者,至少具备以下条件之一:多发性黑色素瘤(≥3个);个人/家族有胰腺癌(PC)病史(最多2级亲属);≥2个一级亲属患有黑色素瘤;≥1个一级亲属患有早发黑色素瘤(结果:≥2个一级亲属患有黑色素瘤;≥1个一级亲属患有早发黑色素瘤;≥1个一级亲属患有早发黑色素瘤):在研究期间,1320 名患者中有 35 人(2.7%)接受了基因检测。4名患者(11.4%)携带黑色素瘤易感基因的PV,其中3人携带CDKN2A基因的PV(8.6%),1人携带MITF基因的PV(2.9%)。CDKN2A(1 例)、MITF(1 例)和 ATM(2 例)中的变异目前被归类为临床意义不明(VUS)。PC和≥5个黑色素瘤的家族史、≥50个痣的个人史以及≥4个黑色素瘤与检测基因中的PV显著相关(P<0.05):结论:FM患者易感基因中PV的发生率低于之前意大利登记处的报告。可能的原因包括未检测的中/低风险基因或尚未发现的高风险基因中的有害变异以及环境风险因素。PC家族史、大量痣和黑色素瘤预示着黑色素瘤的单基因易感性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Prevalence of CDKN2A, CDK4, POT1, BAP1, MITF, ATM, and TERT Pathogenic Variants in a Single-Center Retrospective Series of Patients With Melanoma and Personal or Family History Suggestive of Genetic Predisposition.

Introduction: Approximately 20%-45% of familial melanoma (FM) cases are associated with genetic predisposition.

Objectives: This single-center retrospective study aimed to assess the frequency of pathogenic variants (PV) in the main melanoma-predisposing genes in patients with cutaneous melanoma and investigate the clinical predictors of genetic predisposition.

Methods: Patients included were those diagnosed with cutaneous melanoma at the Dermatology Unit of the University Hospital of Verona, Italy, from 2000 to 2022, presenting at least one of the followings: multiple melanomas (≥ 3); personal/family history of pancreatic cancer (PC) (up to 2nd-degree relatives); ≥ 2 1st-degree relatives with melanoma; ≥ 1 1st-degree relatives with early-onset (<45 years) melanoma and tested for CDKN2A, CDK4, POT1, BAP1, MITF, ATM, and TERT.

Results: During the study period, 35 out of 1320 patients (2.7%) underwent genetic testing. Four patients (11.4%) harbored a PV in a melanoma-predisposing gene, three in CDKN2A (8.6%), and one in MITF (2.9%). Variants currently classified as being of unknown clinical significance (VUS) were detected in CDKN2A (N = 1), MITF (N = 1), and ATM (N = 2). Family history of PC and ≥5 melanomas, personal history of ≥50 nevi, and ≥4 melanomas were significantly associated with PV in tested genes (P < 0.05).

Conclusions: The prevalence of PV in predisposing genes in FM was lower than previously reported in Italian registries. Possible reasons include deleterious variants in untested intermediate/low-penetrance genes or yet-to-be-discovered high-penetrance genes and environmental risk factors. A family history of PC, a high number of nevi and melanomas predict a monogenic predisposition to melanoma.

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