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Molecular characterisation of the 22q13 deletion syndrome supports the role of haploinsufficiency of SHANK3/PROSAP2 in the major neurological symptoms.22q13缺失综合征的分子特征支持SHANK3/PROSAP2单倍剂量不足在主要神经症状中的作用。
J Med Genet. 2003 Aug;40(8):575-84. doi: 10.1136/jmg.40.8.575.
2
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Interaction of G-protein-coupled receptors with synaptic scaffolding proteins.G蛋白偶联受体与突触支架蛋白的相互作用。
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FISH-mapping of a 100-kb terminal 22q13 deletion.22号染色体长臂13区末端100千碱基缺失的荧光原位杂交定位
Hum Genet. 2002 May;110(5):439-43. doi: 10.1007/s00439-002-0713-7. Epub 2002 Apr 4.
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ProSAP/Shank proteins - a family of higher order organizing molecules of the postsynaptic density with an emerging role in human neurological disease.ProSAP/Shank蛋白——一类突触后致密区的高阶组织分子,在人类神经疾病中发挥着越来越重要的作用。
J Neurochem. 2002 Jun;81(5):903-10. doi: 10.1046/j.1471-4159.2002.00931.x.
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No evidence for submicroscopic 22qter deletions in patients with features suggestive for Angelman syndrome.没有证据表明具有疑似安吉尔曼综合征特征的患者存在亚微观的22q末端缺失。
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Study of 250 children with idiopathic mental retardation reveals nine cryptic and diverse subtelomeric chromosome anomalies.对250名特发性智力迟钝儿童的研究发现了9种隐匿且多样的亚端粒染色体异常。
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Subtelomeric rearrangements detected in patients with idiopathic mental retardation.在特发性智力障碍患者中检测到的亚端粒重排。
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Subtelomeric rearrangements: results from a study of selected and unselected probands with idiopathic mental retardation and control individuals by using high-resolution G-banding and FISH.亚端粒重排:一项通过高分辨率G显带和荧光原位杂交技术对特发性智力障碍的选定和未选定先证者及对照个体进行研究的结果。
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Scanning for telomeric deletions and duplications and uniparental disomy using genetic markers in 120 children with malformations.利用基因标记对120名畸形儿童进行端粒缺失、重复及单亲二体扫描。
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22q13缺失综合征的分子特征支持SHANK3/PROSAP2单倍剂量不足在主要神经症状中的作用。

Molecular characterisation of the 22q13 deletion syndrome supports the role of haploinsufficiency of SHANK3/PROSAP2 in the major neurological symptoms.

作者信息

Wilson H L, Wong A C C, Shaw S R, Tse W-Y, Stapleton G A, Phelan M C, Hu S, Marshall J, McDermid H E

机构信息

Department of Biological Sciences, University of Alberta, Edmonton, Alberta T6G 2E9, Canada.

出版信息

J Med Genet. 2003 Aug;40(8):575-84. doi: 10.1136/jmg.40.8.575.

DOI:10.1136/jmg.40.8.575
PMID:12920066
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1735560/
Abstract

METHODS

The 22q13 deletion syndrome (MIM 606232) is characterised by moderate to profound mental retardation, delay/absence of expressive speech, hypotonia, normal to accelerated growth, and mild dysmorphic features. We have determined the deletion size and parent of origin in 56 patients with this syndrome.

RESULTS

Similar to other terminal deletion syndromes, there was an overabundance of paternal deletions. The deletions vary widely in size, from 130 kb to over 9 Mb; however all 45 cases that could be specifically tested for the terminal region at the site of SHANK3 were deleted for this gene. The molecular structure of SHANK3 was further characterised. Comparison of clinical features to deletion size showed few correlations. Some measures of developmental assessment did correlate to deletion size; however, all patients showed some degree of mental retardation and severe delay or absence of expressive speech, regardless of deletion size.

CONCLUSION

Our analysis therefore supports haploinsufficiency of the gene SHANK3, which codes for a structural protein of the postsynaptic density, as a major causative factor in the neurological symptoms of 22q13 deletion syndrome.

摘要

方法

22q13缺失综合征(MIM 606232)的特征为中度至重度智力发育迟缓、语言表达延迟/缺失、肌张力减退、生长正常或加速以及轻度畸形特征。我们确定了56例该综合征患者的缺失大小和起源亲本。

结果

与其他末端缺失综合征相似,父系缺失过多。缺失大小差异很大,从130 kb到超过9 Mb;然而,在SHANK3位点可对末端区域进行特异性检测的所有45例患者中,该基因均缺失。对SHANK3的分子结构进行了进一步表征。临床特征与缺失大小的比较显示相关性很少。一些发育评估指标确实与缺失大小相关;然而,无论缺失大小如何,所有患者均表现出一定程度的智力发育迟缓以及严重的语言表达延迟或缺失。

结论

因此,我们的分析支持编码突触后致密结构蛋白的SHANK3基因单倍剂量不足是22q13缺失综合征神经症状的主要致病因素。