Whole-exome analysis of a Li–Fraumeni family trio with a novel TP53 PRD mutation and anticipation profile

先证者 遗传学 外显子组测序 移码突变 李-弗劳门尼综合征 外显子组 桑格测序 错义突变 无义突变 生物 预测(人工智能) 种系突变 突变 基因 计算机科学 人工智能
作者
Sara Franceschi,Laura Spugnesi,Paolo Aretini,Francesca Lessi,Rosa Scarpitta,Alvaro Galli,Caterina Congregati,Maria A. Caligo,Chiara Maria Mazzanti
出处
期刊:Carcinogenesis [Oxford University Press]
卷期号:38 (9): 938-943 被引量:13
标识
DOI:10.1093/carcin/bgx069
摘要

Li-Fraumeni syndrome is a clinically heterogeneous familial cancer predisposition syndrome with autosomal-dominant inheritance caused by heterozygous germline mutations in the TP53 gene. We here analyze the genetic background of a family with a 4-year-proband presented with a Li-Fraumeni tumor. The mother developed breast cancer at age 37 and the proband died at age 8. We performed Sanger sequencing and whole-exome sequencing on peripheral blood DNA from proband and relatives. Data analysis selected only high-quality score and depth reads, rare variants and protein impact involving missense, non-sense, frameshift and splice disrupt mutations. Disease implicated variants and predicted deleterious alterations were also chosen. TP53 genetic testing revealed a never reported TP53 deletion arose as de novo mutation in the mother and inherited by the proband. We then performed whole-exome analysis of the trio to uncover inherited variants from the father that potentially worsen the already altered genetic background in the proband. No pathogenic variants were inherited in autosomal recessive, de novo dominant or X-linked recessive manner. Comparing proband and father exome we detected 25 predicted deleterious variants including a nonsense mutation in ERCC3. Those inherited mutations are possible candidate modifiers linked to TP53, explaining the proband accelerated tumor onset compared to the mother and providing a possible explanation of the genetic anticipation event in this Li-Fraumeni family.

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