Department of Hematology and Oncology of Children's Medical Center, Hunan Provincial People's Hospital/The First Affiliated Hospital of Hunan Normal University, Changsha, Hunan 410005, P.R. China.
Mol Med Rep. 2017 Nov;16(5):6526-6531. doi: 10.3892/mmr.2017.7416. Epub 2017 Aug 31.
Wiskott‑Aldrich syndrome (WAS) is a rare X‑linked recessive immunodeficiency disorder, characterized by thrombocytopenia, small platelets, eczema and recurrent infections associated with increased risk of autoimmunity and malignancy disorders. Mutations in the WAS protein (WASP) gene are responsible for WAS. To date, WASP mutations, including missense/nonsense, splicing, small deletions, small insertions, gross deletions, and gross insertions have been identified in patients with WAS. In addition, WASP‑interacting proteins are suspected in patients with clinical features of WAS, in whom the WASP gene sequence and mRNA levels are normal. The present study aimed to investigate the application of next generation sequencing in definitive diagnosis and clinical therapy for WAS. A 5 month‑old child with WAS who displayed symptoms of thrombocytopenia was examined. Whole exome sequence analysis of genomic DNA showed that the coverage and depth of WASP were extremely low. Quantitative polymerase chain reaction indicated total WASP gene deletion in the proband. In conclusion, high throughput sequencing is useful for the verification of WAS on the genetic profile, and has implications for family planning guidance and establishment of clinical programs.
威特综合征(Wiskott-Aldrich syndrome,WAS)是一种罕见的 X 连锁隐性免疫缺陷病,其特征为血小板减少、血小板体积小、湿疹和复发性感染,同时伴有自身免疫和恶性疾病的风险增加。WAS 蛋白(WASP)基因突变导致 WAS。迄今为止,已在 WAS 患者中发现 WASP 基因突变,包括错义/无义、剪接、小缺失、小插入、大片段缺失和大片段插入。此外,在具有 WAS 临床特征但 WASP 基因序列和 mRNA 水平正常的患者中,怀疑存在 WASP 相互作用蛋白。本研究旨在探讨下一代测序技术在 WAS 明确诊断和临床治疗中的应用。对一名 5 月龄表现为血小板减少症的 WAS 患儿进行检查。对基因组 DNA 进行全外显子组序列分析显示,WASP 的覆盖度和深度极低。定量聚合酶链反应显示先证者存在 WASP 基因完全缺失。总之,高通量测序有助于在遗传谱上对 WAS 进行验证,对计划生育指导和临床方案的建立具有重要意义。
