患有癌症和先天性异常的儿科患者中癌症易感基因的种系突变。
Germline mutations in cancer predisposition genes among pediatric patients with cancer and congenital anomalies.
作者信息
Dangoni Gustavo D, Teixeira Anne Caroline B, da Costa Silvia S, Scliar Marília O, Carvalho Laura M L, Silva Luciana N, Novak Estela M, Vince Carolina S C, Maschietto Mariana C, Sugayama Sofia M M, Odone-Filho Vicente, Krepischi Ana Cristina V
机构信息
Human Genome and Stem Cell Research Center, Department of Genetics and Evolutionary Biology, Institute of Biosciences, University of São Paulo, São Paulo, SP, Brazil.
Department of Pediatrics, Instituto de Tratamento do Câncer Infantil (ITACI), Faculty of Medicine, University of São Paulo, São Paulo, SP, Brazil.
出版信息
Pediatr Res. 2024 Apr;95(5):1346-1355. doi: 10.1038/s41390-023-03000-7. Epub 2024 Jan 5.
BACKGROUND
Childhood cancer has a poorly known etiology, and investigating the underlying genetic background may provide novel insights. A recognized association exists between non-chromosomal birth defects and childhood cancer susceptibility.
METHODS
We performed whole-exome sequencing and chromosomal microarray analysis in a cohort of childhood cancer (22 individuals, 50% with congenital anomalies) to unravel deleterious germline variants.
RESULTS
A diagnostic yield of 14% was found, encompassing heterozygous variants in bona fide dominant Cancer Predisposition Genes (CPGs). Considering candidate and recessive CPGs harboring monoallelic variants, which were also deemed to play a role in the phenotype, the yield escalated to 45%. Most of the deleterious variants were mapped in genes not conventionally linked to the patient's tumor type. Relevant findings were detected in 55% of the syndromic individuals, mostly variants potentially underlying both phenotypes.
CONCLUSION
We uncovered a remarkable prevalence of germline deleterious CPG variants, highlighting the significance of a comprehensive genetic analysis in pediatric cancer, especially when coupled with additional clinical signs. Moreover, our findings emphasized the potential for oligogenic inheritance, wherein multiple genes synergistically increase cancer risk. Lastly, our investigation unveiled potentially novel genotype-phenotype associations, such as SETD5 in neuroblastoma, KAT6A in gliomas, JAG1 in hepatoblastomas, and TNFRSF13B in Langerhans cell histiocytosis.
IMPACT
Novel gene-phenotype associations and candidate genes for pediatric cancer were unraveled, such as KAT6A in gliomas, SETD5 in neuroblastoma, JAG1 in hepatoblastomas, and TNFRSF13B in Langerhans cell histiocytosis. Our analysis revealed a high frequency of deleterious germline variants, particularly in cases accompanied by additional clinical signs, highlighting the importance of a comprehensive genetic evaluation in childhood cancer. Our findings also underscored the potential for oligogenic inheritance in pediatric cancer risk. Understanding the cancer etiology is crucial for genetic counseling, often influencing therapeutic decisions and offering valuable insights into molecular targets for the development of oncological therapies.
背景
儿童癌症的病因鲜为人知,研究其潜在的遗传背景可能会提供新的见解。非染色体出生缺陷与儿童癌症易感性之间存在公认的关联。
方法
我们对一组儿童癌症患者(22例个体,50%有先天性异常)进行了全外显子组测序和染色体微阵列分析,以揭示有害的种系变异。
结果
诊断率为14%,包括真正的显性癌症易感基因(CPGs)中的杂合变异。考虑到携带单等位基因变异的候选和隐性CPGs,这些变异也被认为在表型中起作用,诊断率升至45%。大多数有害变异位于通常与患者肿瘤类型无关的基因中。在55%的综合征个体中检测到相关发现,大多数变异可能是两种表型的潜在基础。
结论
我们发现种系有害CPG变异的发生率很高,凸显了全面基因分析在儿童癌症中的重要性,特别是当伴有其他临床体征时。此外,我们的研究结果强调了寡基因遗传的可能性,即多个基因协同增加癌症风险。最后,我们的研究揭示了潜在的新的基因型-表型关联,如神经母细胞瘤中的SETD5、胶质瘤中的KAT6A、肝母细胞瘤中的JAG1以及朗格汉斯细胞组织细胞增多症中的TNFRSF13B。
影响
揭示了儿童癌症的新基因-表型关联和候选基因,如胶质瘤中的KAT6A、神经母细胞瘤中的SETD5、肝母细胞瘤中的JAG1以及朗格汉斯细胞组织细胞增多症中的TNFRSF13B。我们的分析显示有害种系变异的频率很高,特别是在伴有其他临床体征的病例中,凸显了儿童癌症全面基因评估的重要性。我们的研究结果还强调了儿童癌症风险中寡基因遗传的可能性。了解癌症病因对于遗传咨询至关重要,通常会影响治疗决策,并为肿瘤治疗开发的分子靶点提供有价值的见解。
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