Constitutional mosaicism of pathogenic variants in SMARCB1 in a subset of patients with sporadic rhabdoid tumors

IF 16.4 1区 医学 Q1 CLINICAL NEUROLOGY
Lara S Fleischmann, Karolina Nemes, Selina Glaser, Alexandra G Kouroukli, Matej Boros, Susanne Bens, Sonja Dahlum, Helene Kretzmer, Florian Oyen, Joachim Gerss, Martin Hasselblatt, Michael C Frühwald, Reiner Siebert
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Abstract

Background Malignant rhabdoid tumors are aggressive malignancies predominantly affecting very young children. The characteristic genetic alteration is biallelic inactivation of SMARCB1. In approximately 30% of patients one SMARCB1 allele is constitutionally altered conferring a particularly unfavourable prognosis. Constitutional mosaicism for pathogenic SMARCB1 mutations has recently been reported in distinct cases of allegedly sporadic rhabdoid tumors. We aimed to systematically investigate the frequency and clinical impact of constitutional mosaicism in patients with sporadic rhabdoid tumors included in the EU-RHAB registry. Methods We selected 29 patients with rhabdoid tumors displaying at least one pathogenic small variant in SMARCB1 in the tumor DNA and absence of a germline mutation. We re-screened blood-derived patient and control DNA for the respective small variant by PCR with unique molecular identifiers and ultra-deep next generation sequencing. Clinical data in patients with and without mosaicism and 174 EU-RHAB controls were compared. Results Employing an ultra-deep sequencing approach, we detected tumor-associated SMARCB1 variants in blood-derived DNA in 9/29 patients. In 6/29 patients (21%), whose variant allele frequency (VAF) exceeded 2%, constitutional mosaicism was assumed whereas tumor DNA contamination was documented in 1/3 patients with VAF below 1%. No significant differences were observed between 6 mosaic-positive and 20 -negative patients regarding age at diagnosis, presence of metastases, event-free or overall survival. Conclusion Constitutional mosaicism for pathogenic small SMARCB1 variants is recurrent in patients with allegedly sporadic rhabdoid tumors. The clinical implications of such variants need to be determined in larger, prospective cohorts also including detection of structural variants of SMARCB1.
散发性横纹肌瘤患者中SMARCB1致病性变异的宿主镶嵌现象
背景 恶性横纹肌瘤是一种侵袭性恶性肿瘤,主要影响年幼儿童。其特征性基因改变是 SMARCB1 的双等位基因失活。约 30% 的患者中,有一个 SMARCB1 等位基因发生了体质性改变,预后特别差。最近有报道称,在不同的所谓散发性横纹肌瘤病例中存在致病性SMARCB1突变的体质镶嵌现象。我们的目的是系统地研究欧盟横纹肌瘤登记处收录的散发性横纹肌瘤患者中出现致病基因嵌合的频率及其临床影响。方法 我们选择了 29 例横纹肌瘤患者,这些患者的肿瘤 DNA 中至少有一个 SMARCB1 致病性小变异,且不存在种系突变。我们通过带有独特分子识别码的 PCR 和超深度新一代测序,重新筛查了患者和对照组血源性 DNA 中的相应小变异。比较了有马赛克和无马赛克患者的临床数据以及 174 例欧盟-RHAB 对照组的临床数据。结果 通过超深度测序方法,我们在 9/29 例患者的血源性 DNA 中检测到了肿瘤相关的 SMARCB1 变异。在变异等位基因频率(VAF)超过 2% 的 6/29 例患者(21%)中,假定存在宪制嵌合,而在 VAF 低于 1% 的 1/3 例患者中,记录到了肿瘤 DNA 污染。在诊断时的年龄、有无转移、无事件生存期或总生存期方面,6 名马赛克阳性患者与 20 名阴性患者之间没有明显差异。结论 在据称是散发性横纹肌瘤的患者中,致病性 SMARCB1 小变体的宪制镶嵌现象反复出现。此类变异的临床影响需要在更大规模的前瞻性队列中确定,其中也包括对SMARCB1结构变异的检测。
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来源期刊
Neuro-oncology
Neuro-oncology 医学-临床神经学
CiteScore
27.20
自引率
6.30%
发文量
1434
审稿时长
3-8 weeks
期刊介绍: Neuro-Oncology, the official journal of the Society for Neuro-Oncology, has been published monthly since January 2010. Affiliated with the Japan Society for Neuro-Oncology and the European Association of Neuro-Oncology, it is a global leader in the field. The journal is committed to swiftly disseminating high-quality information across all areas of neuro-oncology. It features peer-reviewed articles, reviews, symposia on various topics, abstracts from annual meetings, and updates from neuro-oncology societies worldwide.
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