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一名患有综合征性智力障碍患者 2p11.2 间质微重复:30 年随访

Interstitial microduplication at 2p11.2 in a patient with syndromic intellectual disability: 30-year follow-up.

作者信息

Jun Kyung Ran, Ullmann Reinhard, Khan Saadullah, Layman Lawrence C, Kim Hyung-Goo

机构信息

Department of Laboratory Medicine, Inje University Haeundae Paik Hospital, Busan, South Korea.

Department of Human Molecular Genetics, Max Planck Institute for Molecular Genetics, Berlin, Germany.

出版信息

Mol Cytogenet. 2014 Aug 19;7:52. doi: 10.1186/1755-8166-7-52. eCollection 2014.

DOI:10.1186/1755-8166-7-52
PMID:25295072
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4188067/
Abstract

BACKGROUND

Copy number variations at 2p11.2 have been rare and to our knowledge, no abnormal phenotype with an interstitial 2p11.2 duplication has yet been reported. Here we report the first case with syndromic intellectual disability associated with microduplication at 2p11.2.

RESULTS

We revisited a white female subject with a chromosome translocation, t(8;10)(p23;q23)mat and a 10q telomeric deletion suspected by G-banding 30 years ago. This female with severe intellectual disability, no speech, facial dysmorphism, intractable epilepsy, recurrent infection, and skeletal abnormalities has been observed from the birth until her death. The karyotype analysis reconfirmed the previously reported chromosome translocation with a revision as 46,XX,t(8;10)(p23.3;q23.2)mat by adding more detail in chromosomal sub-bands. The array comparative genomic hybridization, however, did not detect the 10q terminal deletion originally reported, but instead, revealed a 390 kb duplication at 2p11.2; 46,XX,t(8;10)(p23.3;q23.2)mat.arr[hg 19] 2p11.2(85469151x2,85474356-85864257x3,85868355x2). This duplication region was confirmed by real-time quantitative PCR and real-time reverse transcriptase quantitative PCR.

CONCLUSIONS

We suggest three positional candidate genes for intellectual disability and recurrent infection based upon gene function and data from real-time reverse transcriptase quantitative PCR-VAMP8 and RNF181 for intellectual disability and CAPG for recurrent infection.

摘要

背景

2p11.2处的拷贝数变异较为罕见,据我们所知,尚未有关于间质性2p11.2重复导致异常表型的报道。在此,我们报告首例与2p11.2微重复相关的综合征性智力障碍病例。

结果

我们重新评估了一名30年前经G显带怀疑存在染色体易位t(8;10)(p23;q23)mat和10q端粒缺失的白人女性患者。该女性自出生直至死亡期间,一直存在严重智力障碍、无语言能力、面部畸形、难治性癫痫、反复感染及骨骼异常。核型分析再次确认了先前报道的染色体易位,并通过在染色体亚带添加更多细节将其修订为46,XX,t(8;10)(p23.3;q23.2)mat。然而,阵列比较基因组杂交未检测到最初报道的10q末端缺失,而是发现了2p11.2处390 kb的重复;46,XX,t(8;10)(p23.3;q23.2)mat.arr[hg 19] 2p11.2(85469151x2,85474356 - 85864257x3,85868355x2)。该重复区域通过实时定量PCR和实时逆转录定量PCR得到确认。

结论

基于基因功能及实时逆转录定量PCR的数据,我们提出三个与智力障碍和反复感染相关的定位候选基因——与智力障碍相关的VAMP8和RNF181,以及与反复感染相关的CAPG。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11e5/4188067/07eddf83c9e4/1755-8166-7-52-2.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11e5/4188067/c79659c817de/1755-8166-7-52-1.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11e5/4188067/07eddf83c9e4/1755-8166-7-52-2.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11e5/4188067/c79659c817de/1755-8166-7-52-1.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11e5/4188067/07eddf83c9e4/1755-8166-7-52-2.jpg

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