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儿童脑瘤患者的遗传易感性和进化痕迹:前瞻性 5 年基于人群的全基因组测序研究。

Genetic predisposition and evolutionary traces of pediatric cancer risk: a prospective 5-year population-based genome sequencing study of children with CNS tumors.

机构信息

Department of Pediatrics and Adolescent Medicine, Rigshospitalet - Copenhagen University Hospital, Copenhagen, Denmark.

Department of Clinical Genetics, Rigshospitalet - Copenhagen University Hospital, Copenhagen, Denmark.

出版信息

Neuro Oncol. 2023 Apr 6;25(4):761-773. doi: 10.1093/neuonc/noac187.

DOI:10.1093/neuonc/noac187
PMID:35902210
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10076945/
Abstract

BACKGROUND

The etiology of central nervous system (CNS) tumors in children is largely unknown and population-based studies of genetic predisposition are lacking.

METHODS

In this prospective, population-based study, we performed germline whole-genome sequencing in 128 children with CNS tumors, supplemented by a systematic pedigree analysis covering 3543 close relatives.

RESULTS

Thirteen children (10%) harbored pathogenic variants in known cancer genes. These children were more likely to have medulloblastoma (OR 5.9, CI 1.6-21.2) and develop metasynchronous CNS tumors (P = 0.01). Similar carrier frequencies were seen among children with low-grade glioma (12.8%) and high-grade tumors (12.2%). Next, considering the high mortality of childhood CNS tumors throughout most of human evolution, we explored known pediatric-onset cancer genes, showing that they are more evolutionarily constrained than genes associated with risk of adult-onset malignancies (P = 5e-4) and all other genes (P = 5e-17). Based on this observation, we expanded our analysis to 2986 genes exhibiting high evolutionary constraint in 141,456 humans. This analysis identified eight directly causative loss-of-functions variants, and showed a dose-response association between degree of constraint and likelihood of pathogenicity-raising the question of the role of other highly constrained gene alterations detected.

CONCLUSIONS

Approximately 10% of pediatric CNS tumors can be attributed to rare variants in known cancer genes. Genes associated with high risk of childhood cancer show evolutionary evidence of constraint.

摘要

背景

儿童中枢神经系统(CNS)肿瘤的病因在很大程度上尚不清楚,并且缺乏基于人群的遗传易感性研究。

方法

在这项前瞻性、基于人群的研究中,我们对 128 名 CNS 肿瘤患儿进行了种系全基因组测序,并通过涵盖 3543 名近亲的系统家系分析进行了补充。

结果

13 名儿童(10%)携带已知癌症基因的致病性变异。这些儿童更有可能患有髓母细胞瘤(OR 5.9,95%CI 1.6-21.2),并且更有可能发生同时性 CNS 肿瘤(P=0.01)。在低级别胶质瘤患儿(12.8%)和高级别肿瘤患儿(12.2%)中也观察到类似的携带率。接下来,考虑到儿童 CNS 肿瘤在人类进化的大部分时间内的高死亡率,我们探索了已知的儿科发病癌症基因,发现它们比与成人发病恶性肿瘤风险相关的基因(P=5e-4)和所有其他基因(P=5e-17)受到更强的进化约束。基于这一观察结果,我们将分析扩展到了 141456 名人类中表现出高进化约束的 2986 个基因。该分析确定了 8 个直接因果关系的功能丧失变异,并且显示了约束程度与致病性提高之间的剂量反应关系,提出了其他高度约束基因改变的作用问题。

结论

大约 10%的儿童 CNS 肿瘤可归因于已知癌症基因的罕见变异。与儿童癌症高风险相关的基因显示出进化约束的证据。

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