多焦点遗传性肿瘤等位基因综合征:关于 CHEK2/ATM 和 BRCA1/CDKN2A 基因之间不常见组合的报告

IF 1.2 Q4 ONCOLOGY ecancermedicalscience Pub Date : 2024-05-10 DOI:10.3332/ecancer.2024.1701
Ricardo Ubilla, Michelle Zeppelin, Fernanda Martin
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摘要

背景:多病灶遗传性肿瘤等位基因综合征(MINAS)是最近创造的一个术语,它描述了癌症易感基因(CSGs)中两个或两个以上致病变体(PVs)同时存在于一个人体内的情况。病例介绍:本文介绍了两例因罕见的 CSG 组合而导致的 MINAS 病例。第一个病例是一名 37 岁的女性,她的共济失调性毛细血管扩张症(ATM)和 CHEK2 基因突变携带 PV,29 岁时患上 HER-2 阳性的单侧乳腺癌。第二名患者是一名 53 岁女性,携带 BRCA1 和 CDKN2A 基因的 PV,51 岁时患上三阴性乳腺癌。我们介绍了她们的家族病史和治疗情况,其中个性化管理证据的缺乏显而易见。结论预测携带 CSG 两个变体的表型效应具有挑战性。必须鼓励通报其他病例并开展功能研究,以确定受影响个体的特定风险,从而制定个性化的随访指南,降低相关的死亡率。
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Multilocus inherited neoplasia allele syndrome: report of uncommon combinations between CHEK2/ATM and BRCA1/CDKN2A genes
Background: Multilocus inherited neoplasia allelic syndrome (MINAS) is a recently coined term that describes the coexistence of two or more pathogenic variants (PVs) in cancer susceptibility genes (CSGs) in a single individual. Case presentation: This article presents two cases of MINAS due to rare CSG combinations. The first was a 37-year-old woman carrying PVs in the mutated ataxia telangiec-tasia ( ATM ) and CHEK2 genes, with HER-2 positive unilateral breast cancer at 29. The second was a 53-year-old woman carrying PVs in the BRCA1 and CDKN2A genes, who presented with triple-negative breast cancer at 51. We describe their family history and treatment, where the lack of evidence for personalised management becomes evident. Conclusion: Predicting the phenotypic effect of harbouring two variants in CSG is challenging. It is essential to encourage the notification of other cases and carry out functional studies to establish specific risks for affected individuals to develop personalised follow-up guidelines to reduce the associated morbimortality.
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来源期刊
CiteScore
3.80
自引率
5.60%
发文量
138
审稿时长
27 weeks
期刊最新文献
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