Crowgey Erin L, Soini Tea, Shah Nidhi, Pauniaho Satu-Liisa, Lahdenne Pekka, Wilson David B, Heikinheimo Markku, Druley Todd E
Nemours Center for Cancer and Blood Disorders, Nemours Alfred I. duPont Hospital for Children, Wilmington, DE, USA.
Pediatric Research Center, Children's Hospital, University of Helsinki and Helsinki University Hospital, Helsinki, Finland.
Appl Clin Genet. 2020 Jun 30;13:127-137. doi: 10.2147/TACG.S245093. eCollection 2020.
Pediatric germ cell tumors are rare, representing about 3% of childhood malignancies in children less than 15 years of age, presenting in neonates or adolescents with a greater incidence noted in older adolescents. Aberrations in primordial germ cell proliferation/differentiation can lead to a variety of neoplasms, including teratomas, embryonal carcinoma, choriocarcinoma, and yolk sac tumors.
Three Finnish families with varying familial germ cell tumors were identified, and whole-genome sequencing was performed using an Illumina sequencing platform. In total, 22 unique subjects across the three families were sequenced. Family 1 proband (female) was affected by malignant ovarian teratoma, Family 2 proband (female) was affected by sacrococcygeal teratoma with yolk sac tumor in the setting of Cornelia de Lange syndrome, and Family 3 proband (male) was affected by malignant testicular teratoma. Rare variants were identified using an autosomal recessive or de novo model of inheritance.
For family 1 proband (female), an autosomal recessive or de novo model of inheritance identified variants of interest in the following genes: , and . Family 2 proband (female) analysis identified gene variants of interest in the following genes: . Family 3 proband (male) analysis identified the following potential genes: , and .
Leveraging deep pedigrees and next-generation sequencing, rare germline variants were identified that were enriched in three families from Finland with a history of familial germ cell tumors. The data presented support the importance of germline mutations when analyzing complex cancers with a low somatic mutation landscape.
小儿生殖细胞肿瘤较为罕见,在15岁以下儿童的儿童期恶性肿瘤中约占3%,在新生儿或青少年中发病,年龄较大的青少年发病率更高。原始生殖细胞增殖/分化异常可导致多种肿瘤,包括畸胎瘤、胚胎癌、绒毛膜癌和卵黄囊瘤。
确定了三个患有不同家族性生殖细胞肿瘤的芬兰家庭,并使用Illumina测序平台进行全基因组测序。三个家庭共有22名独特个体接受了测序。家族1的先证者(女性)患有恶性卵巢畸胎瘤,家族2的先证者(女性)患有骶尾部畸胎瘤并伴有卵黄囊瘤,同时患有科妮莉亚·德朗热综合征,家族3的先证者(男性)患有恶性睾丸畸胎瘤。使用常染色体隐性遗传或新发遗传模型鉴定罕见变异。
对于家族1的先证者(女性),常染色体隐性遗传或新发遗传模型在以下基因中鉴定出了感兴趣的变异: ,以及 。家族2先证者(女性)的分析在以下基因中鉴定出了感兴趣的基因变异: 。家族3先证者(男性)的分析鉴定出了以下潜在基因: ,以及 。
利用深度家系和下一代测序技术,在芬兰三个有家族性生殖细胞肿瘤病史的家庭中鉴定出了罕见的种系变异。所呈现的数据支持在分析体细胞突变情况较少的复杂癌症时种系突变的重要性。
