常染色体隐性遗传性智力残疾家庭的遗传分析

IF 0.5 Q3 MEDICINE, GENERAL & INTERNAL Gomal Journal of Medical Sciences Pub Date : 2019-06-30 DOI:10.46903/17.02.1908
Jamshed Khan, M. Junaid, S. Uddin, K. Moeed, Usman Ullah, Shehla Aman
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引用次数: 0

摘要

背景:智力残疾是一种神经发育缺陷,表现为发育迟缓和学习障碍。这种缺陷可能是由染色体疾病(18三体或唐氏综合症)或单基因突变引起的。其全球流行率估计为1-3%。非综合征性ID的遗传病因尚不清楚。迄今为止,已有100多个基因座与非综合征ID相关。本研究的目的是确定三种材料和方法的致病基因:这项横断面研究于2014年3月至2015年8月在巴基斯坦白沙瓦开伯尔医科大学基础医学科学研究所进行。为这些家庭设定的纳入标准是血亲关系,每个家庭有两名以上的患者(包括表亲)。所有患者都在友好的环境中进行了单独测试,使用IQ测试根据表现对ID进行评分。此后,通过无菌方法采集血液样本,并提取DNA以进行遗传分析。在基因分析中,进行外显子组测序以发现致病性变体。随后桑格测序也被用来观察致病性变体的分离。结果:遗传分析发现AP4B1在家族1中发生突变,WDR62在家族2中发生突变。结论:本研究对三个亲缘家族进行了基因分析,发现AP4B1在家族1中发生突变,WDR62在家族2中发生突变。本研究将有助于设计婚前和受孕前检测的分子诊断技术。
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GENETIC ANALYSIS OF FAMILIES HAVING AUTOSOMAL RECESSIVE INTELLECTUAL DISABILITY
Background: Intellectual disability (ID) is a neuro-developmental defect that is manifested by development delay and learning disability. Such defects may be caused due to chromosomal disorders (trisomy 18 or Down syndrome) or single gene mutation. Its worldwide prevalence is estimated to be 1-3%. The genetic etiology of non-syndromic ID is poorly understood. To date, more than 100 loci have been reported to be associated with non-syndromic ID. The objective of this study was to identify the causative genes for three Materials & Methods: This cross-sectional study was conducted in the Institute of Basic Medical Sciences, Khyber Medical University, Peshawar, Pakistan from March 2014 to August 2015. The inclusion criteria set for the families was consanguineous relation and more than two patients per family (including cousins). All the patients were tested individually in friendly atmosphere using IQ test to scale the ID on the basis of performance. Thereafter, blood samples were taken by aseptic method and DNA was extracted for the purpose of doing genetic analysis. In genetic analysis, exome sequencing was performed to find the pathogenic variants. Subsequently. Sanger sequencing was also done to see the segregation of pathogenic variants. Results: Genetic analysis found mutation in AP4B1 in Family 1, in WDR62 in Family 2, while Family 3 was unremarkable. Conclusion: The study involved genetic analysis of three consanguineous families and found mutation in AP4B1 in Family 1, in WDR62 in Family 2, while Family 3 was unremarkable. The present research will help in devising molecular diagnostic technics for pre-marital and pre-conception testing.
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来源期刊
Gomal Journal of Medical Sciences
Gomal Journal of Medical Sciences MEDICINE, GENERAL & INTERNAL-
CiteScore
0.60
自引率
80.00%
发文量
37
审稿时长
40 weeks
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