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神经纤维瘤病诊所中的SPRED 1突变

SPRED 1 mutations in a neurofibromatosis clinic.

作者信息

Muram-Zborovski Talia M, Stevenson David A, Viskochil David H, Dries David C, Wilson Andrew R

机构信息

Department of Pathology, University of Utah, Salt Lake City, Utah, USA.

出版信息

J Child Neurol. 2010 Oct;25(10):1203-9. doi: 10.1177/0883073809359540. Epub 2010 Feb 22.

DOI:10.1177/0883073809359540
PMID:20179001
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3243064/
Abstract

Legius syndrome, caused by SPRED1 mutations, has phenotypic overlap with neurofibromatosis type 1 (NF1) without tumorigenic manifestations. Patients fulfilling the National Institutes of Health (NIH) diagnostic criteria for NF1 were enrolled at the University of Utah NF Clinic, and SPRED1 mutation analysis was performed to identify the frequency of Legius syndrome within an NF1 clinic population. SPRED1 sequencing was performed on 151 individuals with the clinical diagnosis of NF1, and 2 individuals (1.3%) were found to have novel SPRED1 mutations, p.R18X and p.Q194X. The phenotypes for the 2 individuals with SPRED1 mutations included altered pigmentation without tumorigenesis. A specific SPRED1 haplotype allele was identified in 27 individuals. The frequency of SPRED1 mutations in patients meeting diagnostic criteria for NF1 in a hospital-based clinic is 1% to 2%. The likelihood an individual is harboring a SPRED1 mutation increases with age if multiple, nonpigmentary NF1 findings are absent. Legius syndrome patients may benefit from altered medical surveillance.

摘要

由SPRED1突变引起的Legius综合征与1型神经纤维瘤病(NF1)存在表型重叠,但无肿瘤发生表现。符合美国国立卫生研究院(NIH)NF1诊断标准的患者被纳入犹他大学NF诊所,进行SPRED1突变分析以确定Legius综合征在NF1诊所人群中的发生率。对151例临床诊断为NF1的个体进行了SPRED1测序,发现2例个体(1.3%)有新的SPRED1突变,即p.R18X和p.Q194X。这2例携带SPRED1突变个体的表型包括色素沉着改变但无肿瘤发生。在27例个体中鉴定出一种特定的SPRED1单倍型等位基因。在一家医院诊所中,符合NF1诊断标准的患者中SPRED1突变的发生率为1%至2%。如果不存在多个非色素性NF1表现,个体携带SPRED1突变的可能性会随着年龄增长而增加。Legius综合征患者可能会从改变的医学监测中受益。

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