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对南印度散发圆锥角膜患者的VSX1序列变异的研究。

Investigation of VSX1 sequence variants in South Indian patients with sporadic cases of keratoconus.

作者信息

Verma Anshuman, Das Manoranjan, Srinivasan Muthiah, Prajna Namperumalsamy V, Sundaresan Periasamy

机构信息

Department of Genetics, Dr. G. Venkataswamy Eye Research Institute, Aravind Medical Research Foundation, Aravind Eye Hospital, Madurai, Tamil Nadu, India.

出版信息

BMC Res Notes. 2013 Mar 18;6:103. doi: 10.1186/1756-0500-6-103.

Abstract

BACKGROUND

The involvement of VSX1 gene for the genetic basis of keratoconus is unclear and controversial. The genetic screening of VSX1 from different ethnic populations can enlighten this subject. The aim of the present study is to investigate the role of VSX1 gene in patients with sporadic cases of keratoconus from South India.

METHODS

The VSX1 gene coding regions, including exon-intron boundaries were screened by direct sequencing analysis in 117 sporadic cases of keratoconus. The identified variations were also analyzed in 108 ethnic matched healthy blood donors.

RESULTS

In the VSX1 gene screening, no pathogenic mutation was identified, whereas we could find the presence of four reported single nucleotide polymorphisms; c.546A>G (rs12480307), c.627+23G>A (rs6138482), c.627+84T>A (rs56157240) and c.504-24C>T (IVS3-24C). These variations were observed in similar frequency between cases and controls.

CONCLUSIONS

The lack of VSX1 pathogenic variations in a large number of unrelated sporadic keratoconus patients tend to omit its role, and corroborate the involvement of other genetic, environmental or behavioural factors in the development of this complex disorder.

摘要

背景

VSX1基因在圆锥角膜遗传基础中的作用尚不清楚且存在争议。对不同种族人群的VSX1基因进行遗传筛查有助于阐明这一问题。本研究旨在探讨VSX1基因在来自印度南部的散发性圆锥角膜患者中的作用。

方法

通过直接测序分析对117例散发性圆锥角膜患者的VSX1基因编码区(包括外显子-内含子边界)进行筛查。在108名种族匹配的健康献血者中也对鉴定出的变异进行了分析。

结果

在VSX1基因筛查中,未发现致病突变,然而我们发现存在四个已报道的单核苷酸多态性;c.546A>G(rs12480307)、c.627+23G>A(rs6138482)、c.627+84T>A(rs56157240)和c.504-24C>T(IVS3-24C)。这些变异在病例组和对照组中的出现频率相似。

结论

大量无关的散发性圆锥角膜患者中缺乏VSX1致病变异,这倾向于排除其作用,并证实其他遗传、环境或行为因素在这种复杂疾病的发生发展中起作用。

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