儿童特应性皮炎患者的丝聚合蛋白基因突变:对印度基因库的研究,一项初步研究
Filaggrin Gene Mutation in Pediatric Patients with Atopic Dermatitis: A Look into Indian Gene Pool, a Pilot Study.
作者信息
Rajeshwari K A, Thomas Merin M, Nagaraj Geetha
机构信息
From the Department of Dermatology, East Point College of Medical Sciences and Research Centre, Bengaluru, Karnataka, India.
Department of Anatomy, East Point College of Medical Sciences and Research Centre, Bengaluru, Karnataka, India.
出版信息
Indian J Dermatol. 2023 Mar-Apr;68(2):135-140. doi: 10.4103/ijd.ijd_403_22.
BACKGROUND
Mutations in the filaggrin (FLG) gene has been reported to be an indicator of poor prognosis of atopic dermatitis (AD). It has been reported that there is a considerable variation in the mutations detected in the FLG gene in different ethnicities.
AIM
To detect the presence of mutations in the FLG gene in pediatric subjects with atopic dermatitis (AD) and to compare the detected mutations with those already reported from different ethnicities.
MATERIALS AND METHODS
Genomic DNA extracted using standard procedure from peripheral venous blood of 30 patient and 15 control samples. Sequence analysis of the FLG gene carried out and detected changes was then cross referenced with those mutations already reported to check for novelty of detected changes.
RESULTS
Amino acid changes were detected in 28 of the patient samples and in none of the control samples indicating that changes in the FLG gene were more common in the patient group than the control group (Fishers exact test, < 0.0001). The most commonly reported mutations R501X and 2282del4 were not detected. Only 5 of the detected 22 amino acid changes H2507Q, L2481S, K2444E, E2398Q, and S2366T have been previously reported and are not clinically significant; however, in one patient a stop codon was detected (S2366STOP). P2238N, R2239W, and V2243L detected in 70% of the samples and S2231E detected in 67% of the patient samples have not been reported so far and their clinical significance is yet to be analyzed.
CONCLUSION
Analyses of mutations already reported showed that the changes detected from this study are novel to Indian traits. While this adds on to the minimal data available from the Indian subcontinent further analyses has to be carried out to analyze the pathogenicity of these detected changes on larger samples sizes.
AIM
To detect the presence of mutations in the FLG gene in pediatric subjects with atopic dermatitis (AD) and to compare the detected mutations with those already reported from different ethnicities.
背景
据报道,丝聚合蛋白(FLG)基因突变是特应性皮炎(AD)预后不良的一个指标。据报道,在不同种族中检测到的FLG基因突变存在相当大的差异。
目的
检测患有特应性皮炎(AD)的儿科患者中FLG基因突变的存在情况,并将检测到的突变与不同种族中已报道的突变进行比较。
材料与方法
采用标准程序从30例患者的外周静脉血和15例对照样本中提取基因组DNA。对FLG基因进行序列分析,然后将检测到的变化与已报道的那些突变进行交叉对照,以检查检测到的变化是否新颖。
结果
在28例患者样本中检测到氨基酸变化,而在对照样本中均未检测到,这表明FLG基因的变化在患者组中比对照组更常见(Fisher精确检验,<0.0001)。未检测到最常报道的突变R501X和2282del4。在检测到的22种氨基酸变化中,只有5种(H2507Q、L2481S、K2444E、E2398Q和S2366T)先前已被报道且无临床意义;然而,在一名患者中检测到一个终止密码子(S2366STOP)。在70%的样本中检测到的P2238N、R2239W和V2243L以及在67%的患者样本中检测到的S2231E目前尚未见报道,其临床意义有待分析。
结论
对已报道突变的分析表明,本研究检测到的变化对于印度人群特征来说是新的。虽然这增加了来自印度次大陆的极少数据,但还必须进行进一步分析,以在更大样本量上分析这些检测到的变化的致病性。
目的
检测患有特应性皮炎(AD)的儿科患者中FLG基因突变的存在情况,并将检测到的突变与不同种族中已报道的突变进行比较。
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