Germline variants in patients diagnosed with pediatric soft tissue sarcoma.

IF 2.7 3区 医学 Q3 ONCOLOGY
Synnøve Yndestad, Hans Kristian Haugland, Dorota Goplen, Dorota Wojcik, Stian Knappskog, Per Eystein Lønning
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引用次数: 0

Abstract

Background: While soft tissue sarcomas affect younger patients, few studies have assessed the distribution of underlying pathogenic germline variants.

Patients and methods: We retrospectively identified all pediatric and young adult patients (0-22 years) at Haukeland University Hospital, Norway (1981-2019), through clinical and pathological records. We identified n = 46 eligible patients. From these 46 patients, adequate material representing normal tissue was available for n = 41 cases (n = 24 diagnosed with rhabdomyosarcoma, 9 with synovial sarcomas, 2 with Ewing sarcomas, and 6 without further classification), with matching tumor tissue for n = 40. Normal tissue samples were analyzed for germline pathogenic variants (PVs) by targeted sequencing of 360 cancer genes.

Results: Out of the 41 analyzed cases, we found PVs or likely PVs in 7 (17%). These variants were found in TP53, MUTYH, FANCC, DICER1, FANCA, MYO3A, and MYO5B. Supporting the causality of these PVs, four cases revealed loss of heterozygosity (LOH) of the wild-type allele in the tumor tissue, one patient with a PV in DICER1 had a second somatic variant in DICER1, and a patient with a PV in TP53 had the altered allele amplified in the tumor. For three out of five with available family history, a history of other cancers in relatives was recorded. Among genes with variants of uncertain significance, CHD1L was of particular interest, revealing a stop-gain and a missense variant.

Interpretation: A high fraction of young patients with soft tissue sarcoma harbor PVs. Among the genes affected, we substantiate a potential role of MYO5B and propose a potential role for MYO3A.

小儿软组织肉瘤患者的基因变异。
背景:虽然软组织肉瘤影响年轻患者,但很少有研究对潜在致病基因变异的分布进行评估:我们通过临床和病理记录回顾性地确定了挪威豪克兰大学医院的所有儿童和年轻成人患者(0-22 岁)(1981-2019 年)。我们确定了 n = 46 名符合条件的患者。在这 46 名患者中,有 n = 41 例(n = 24 例诊断为横纹肌肉瘤,9 例诊断为滑膜肉瘤,2 例诊断为尤文肉瘤,6 例未进一步分类)获得了代表正常组织的充足材料,n = 40 例获得了匹配的肿瘤组织。通过对 360 个癌症基因进行靶向测序,对正常组织样本的种系致病变体(PVs)进行了分析:在分析的 41 个病例中,我们发现了 7 个病例(17%)存在 PV 或可能存在 PV。这些变异出现在 TP53、MUTYH、FANCC、DICER1、FANCA、MYO3A 和 MYO5B 中。为支持这些变异的因果关系,4 例患者的肿瘤组织中发现了野生型等位基因的杂合性缺失(LOH),1 例 DICER1 变异的患者在 DICER1 中发现了第二个体细胞变异,1 例 TP53 变异的患者在肿瘤中扩增了改变的等位基因。在五名有家族史的患者中,有三名患者的亲属曾患其他癌症。在意义不确定的变异基因中,CHD1L尤其引人关注,它发现了一个终止增益变异和一个错义变异:解释:软组织肉瘤的年轻患者中有很大一部分携带PV。在受影响的基因中,我们证实了 MYO5B 的潜在作用,并提出了 MYO3A 的潜在作用。
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来源期刊
Acta Oncologica
Acta Oncologica 医学-肿瘤学
CiteScore
4.30
自引率
3.20%
发文量
301
审稿时长
3 months
期刊介绍: Acta Oncologica is a journal for the clinical oncologist and accepts articles within all fields of clinical cancer research. Articles on tumour pathology, experimental oncology, radiobiology, cancer epidemiology and medical radio physics are also welcome, especially if they have a clinical aim or interest. Scientific articles on cancer nursing and psychological or social aspects of cancer are also welcomed. Extensive material may be published as Supplements, for which special conditions apply.
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