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脊髓性肌萎缩症分子诊断的临床应用:神经元凋亡抑制蛋白和生存运动神经元基因的缺失

Clinical application of the molecular diagnosis of spinal muscular atrophy: deletions of neuronal apoptosis inhibitor protein and survival motor neuron genes.

作者信息

Somerville M J, Hunter A G, Aubry H L, Korneluk R G, MacKenzie A E, Surh L C

机构信息

Department of Genetics, Children's Hospital of Eastern Ontario, Canada.

出版信息

Am J Med Genet. 1997 Mar 17;69(2):159-65.

PMID:9056553
Abstract

The molecular genetic diagnosis of spinal muscular atrophy (SMA) has recently been complicated by the identification of two candidate genes, which are often deleted in affected individuals but are also occasionally deleted in apparently unaffected carriers. We present a compilation of genotypes, from our laboratory and recent reports, for the survival motor neuron (SMN) and neuronal apoptosis inhibitor protein (NAIP) genes. Bayesian analyses were used to generate probabilities for SMA when deletions are present or absent in SMN. We found that when the SMN(T) exon 7 is deleted, the probability of SMA can reach greater than 98% in some populations, and when SMN(T) is present, the probability of SMA is approximately 17 times less than the prior population risk. Deletion of NAIP exon 5, as well as SMN(T) exon 7, is associated with a 5-fold increased risk of type I SMA. Case studies are used to illustrate differing disease risks for pre- and postnatal testing, depending on the presence of information about clinical status or molecular results. These analyses demonstrate that deletion screening of candidate genes can be a powerful tool in the diagnosis of SMA.

摘要

最近,脊髓性肌萎缩症(SMA)的分子遗传学诊断因发现两个候选基因而变得复杂,这两个基因在受影响个体中常被缺失,但在明显未受影响的携带者中也偶尔会被缺失。我们汇总了来自我们实验室及近期报告中的生存运动神经元(SMN)和神经元凋亡抑制蛋白(NAIP)基因的基因型。当SMN存在或不存在缺失时,采用贝叶斯分析来生成SMA的概率。我们发现,当SMN(T)外显子7缺失时,在某些人群中SMA的概率可达到98%以上,而当SMN(T)存在时,SMA的概率比先前人群风险低约17倍。NAIP外显子5以及SMN(T)外显子7的缺失与I型SMA风险增加5倍相关。案例研究用于说明产前和产后检测的不同疾病风险,这取决于是否存在临床状态或分子结果方面的信息。这些分析表明,候选基因的缺失筛查可以成为SMA诊断中的有力工具。

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