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Analysis of clinical and molecular characteristics of Wiskott-Aldrich syndrome in 24 patients from 23 unrelated Chinese families

机译:来自中国23个无关家庭的24例Wiskott-Aldrich综合征的临床和分子特征分析

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摘要

The clinical data of 24 children with Wiskott-Aldrich syndrome (WAS) from 23 unrelated Chinese families were reviewed in the present study. WAS protein (WASP) expression in peripheral blood mononuclear cells was examined by flow cytometry (FCM); WASP gene was amplified by PCR and directly sequenced to analyze mutations in the WASP gene in patients and their female relatives. FCM analysis of 21 patients showed that 18 cases were WASP-negative, and three had partially WASP expression. WASP gene analysis revealed mutations in 23 patients, including five missense mutations, four nonsense mutations, four deletion mutations, three insertion mutations, six splice site mutations, and one complex mutation, among which, 20 unique mutations were detected, including seven novel mutations (168 C>A, 747-748del T, 793-797del C, 1185 ins C, Dup 1251-1267, 1277 insA and 1266 C>G; 1267-1269del C). Five WAS children underwent stem cell transplantation. After 2 months of transplantation, WASP expression was restored to normal in all five patients whereas one patient died of cytomegalovirus-induced interstitial lung disease. WASP gene analysis can make a definite diagnosis of WAS and identify mutation carriers, beneficial for timely treatment and genetic counseling for children with WAS.
机译:本文对来自23个无关家庭的24例Wiskott-Aldrich综合征(WAS)儿童的临床数据进行了回顾。用流式细胞术(FCM)检测外周血单个核细胞中WAS蛋白(WASP)的表达; WASP基因通过PCR扩增并直接测序以分析患者及其女性亲属中WASP基因的突变。 FCM分析21例患者,其中18例为WASP阴性,三例为WASP部分表达。 WASP基因分析揭示了23例患者的突变,包括5个错义突变,4个无意义突变,4个缺失突变,3个插入突变,6个剪接位点突变和1个复杂突变,其中,检测到20个独特突变,包括7个新突变( 168 C> A,747-748del T,793-797del C,1185 ins C,Dup 1251-1267、1277 insA和1266 C> G; 1267-1269del C)。 5名WAS儿童接受了干细胞移植。移植2个月后,所有5例患者的WASP表达均恢复正常,而1例患者死于巨细胞病毒引起的间质性肺疾病。 WASP基因分析可以对WAS进行明确诊断,并鉴定突变携带者,有利于WAS儿童的及时治疗和遗传咨询。

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