Constitutional balanced translocations involving SMARCB1: A rare cause of rhabdoid tumor predisposition syndrome

IF 3.1 2区 医学 Q2 GENETICS & HEREDITY
Patrick R. Blackburn, Rose B. McGee, Roya Mostafavi, Andrew J. Carroll, Fady M. Mikhail, Gregory T. Armstrong, Larissa V. Furtado, Jason Chiang, David A. Wheeler, Steven S. Carey, Kim E. Nichols, Santhosh A. Upadhyaya
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Abstract

Rhabdoid Tumor Predisposition Syndrome 1 (RTPS1) confers an increased risk of developing rhabdoid tumors and is caused by germline mutations in SMARCB1. RTPS1 should be evaluated in all individuals with rhabdoid tumor and is more likely in those with a young age at presentation (occasionally congenital presentation), multiple primary tumors, or a family history of rhabdoid tumor or RTPS1. Proband genetic testing is the standard method for diagnosing RTPS1. Most known RTPS1-related SMARCB1 gene mutations are copy number variants (CNVs) or single nucleotide variants/indels, but structural variant analysis (SVA) is not usually included in the molecular evaluation. Here, we report two children with RTPS1 presenting with atypical teratoid/rhabdoid tumor (ATRT) who had constitutional testing showing balanced chromosome translocations involving SMARCB1. Patient 1 is a 23-year-old female diagnosed with pineal region ATRT at 7 months who was found to have a de novo, constitutional t(16;22)(p13.3;q11.2). Patient 2 is a 24-month-old male diagnosed with a posterior fossa ATRT at 14 months, with subsequent testing showing a constitutional t(5;22)(q14.1;q11.23). These structural rearrangements have not been previously reported in RTPS1. While rare, these cases suggest that structural variants should be considered in the evaluation of children with rhabdoid tumors to provide more accurate genetic counseling on the risks of developing tumors, the need for surveillance, and the risks of passing the disorder on to future children. Further research is needed to understand the prevalence, clinical features, and tumor risks associated with RTPS1-related constitutional balanced translocations.

涉及 SMARCB1 的体质平衡易位:横纹肌瘤易感综合征的罕见病因
横纹肌瘤易感综合征 1(RTPS1)会增加罹患横纹肌瘤的风险,是由 SMARCB1 的种系突变引起的。所有横纹肌瘤患者都应进行 RTPS1 评估,发病年龄较小(偶尔为先天性发病)、多发性原发性肿瘤或有横纹肌瘤或 RTPS1 家族史的患者更有可能患有 RTPS1。Proband 基因检测是诊断 RTPS1 的标准方法。大多数已知的RTPS1相关SMARCB1基因突变是拷贝数变异(CNV)或单核苷酸变异/indels,但结构变异分析(SVA)通常不包括在分子评估中。在此,我们报告了两名患有 RTPS1 并伴有非典型畸形/横纹肌瘤(ATRT)的儿童,他们的体质检测显示涉及 SMARCB1 的平衡染色体易位。患者1是一名23岁的女性,7个月时被诊断为松果体区ATRT,并发现她有一个新发的常染色体t(16;22)(p13.3;q11.2)。患者 2 是一名 24 个月大的男性,在 14 个月时被诊断出患有后窝 ATRT,随后的检测显示其患有常染色体 t(5;22)(q14.1;q11.23)。这些结构重排以前在 RTPS1 中从未报道过。虽然罕见,但这些病例表明,在对横纹肌瘤患儿进行评估时,应考虑结构变异,以便就患肿瘤的风险、监测的必要性以及将这种疾病遗传给后代的风险提供更准确的遗传咨询。要了解与 RTPS1 相关的宪制平衡易位的发病率、临床特征和肿瘤风险,还需要进一步的研究。
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来源期刊
Genes, Chromosomes & Cancer
Genes, Chromosomes & Cancer 医学-遗传学
CiteScore
7.00
自引率
8.10%
发文量
94
审稿时长
4-8 weeks
期刊介绍: Genes, Chromosomes & Cancer will offer rapid publication of original full-length research articles, perspectives, reviews and letters to the editors on genetic analysis as related to the study of neoplasia. The main scope of the journal is to communicate new insights into the etiology and/or pathogenesis of neoplasia, as well as molecular and cellular findings of relevance for the management of cancer patients. While preference will be given to research utilizing analytical and functional approaches, descriptive studies and case reports will also be welcomed when they offer insights regarding basic biological mechanisms or the clinical management of neoplastic disorders.
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