一个包含SLC1A1基因表达数量性状位点的单倍型及其与强迫症的关联。
A haplotype containing quantitative trait loci for SLC1A1 gene expression and its association with obsessive-compulsive disorder.
作者信息
Wendland Jens R, Moya Pablo R, Timpano Kiara R, Anavitarte Adriana P, Kruse Matthew R, Wheaton Michael G, Ren-Patterson Renee F, Murphy Dennis L
机构信息
Laboratory of Clinical Science, National Institute of Mental Health, National Institutes of Health, Bethesda, MD 20892, USA.
出版信息
Arch Gen Psychiatry. 2009 Apr;66(4):408-16. doi: 10.1001/archgenpsychiatry.2009.6.
CONTEXT
Recent evidence from linkage analyses and follow-up candidate gene studies supports the involvement of SLC1A1, which encodes the neuronal glutamate transporter, in the development of obsessive-compulsive disorder (OCD).
OBJECTIVES
To determine the role of genetic variation of SLC1A1 in OCD in a large case-control study and to better understand how SLC1A1 variation affects functionality.
DESIGN
A case-control study.
SETTING
Publicly accessible SLC1A1 expression and genotype data.
PATIENTS
Three hundred twenty-five OCD probands and 662 ethnically and sex-matched controls.
INTERVENTIONS
Probands were assessed with the Structured Clinical Interview for DSM-IV, the Yale-Brown Obsessive Compulsive Scale, and the Saving Inventory-Revised. Six single-nucleotide polymorphisms (SNPs) were genotyped. Multiple testing corrections for single-marker and haplotype analyses were performed by permutation.
RESULTS
Gene expression of SLC1A1 is heritable in lymphoblastoid cell lines. We identified 3 SNPs in or near SLC1A1 that correlated with gene expression levels, 1 of which had previously been associated with OCD. Two of these SNPs also predicted expression levels in human brain tissue, and 1 SNP was further functional in reporter gene studies. Two haplotypes at 3 SNPs, rs3087879, rs301430, and rs7858819, were significantly associated with OCD after multiple-testing correction and contained 2 SNPs associated with expression levels. In addition, another SNP correlating with SLC1A1 gene expression, rs3933331, was associated with an OCD-hoarding subphenotype as assessed by 2 independent, validated scales.
CONCLUSIONS
Our case-control data corroborate previous smaller family-based studies that indicated that SLC1A1 is a susceptibility locus for OCD. The expression and genotype database-mining approach we used provides a potentially useful complementary approach to strengthen future candidate gene studies in neuropsychiatric and other disorders.
背景
连锁分析和后续候选基因研究的最新证据支持,编码神经元谷氨酸转运体的溶质载体家族1成员1(SLC1A1)参与了强迫症(OCD)的发生发展。
目的
在一项大型病例对照研究中确定SLC1A1基因变异在强迫症中的作用,并更好地了解SLC1A1变异如何影响其功能。
设计
病例对照研究。
研究地点
可公开获取的SLC1A1表达和基因型数据。
患者
325名强迫症先证者和662名种族及性别匹配的对照。
干预措施
采用《精神疾病诊断与统计手册》第四版(DSM-IV)的结构化临床访谈、耶鲁-布朗强迫症量表和修订后的储蓄量表对先证者进行评估。对6个单核苷酸多态性(SNP)进行基因分型。通过排列法对单标记和单倍型分析进行多重检验校正。
结果
SLC1A1的基因表达在淋巴母细胞系中具有遗传性。我们在SLC1A1内部或附近鉴定出3个与基因表达水平相关的SNP,其中1个先前已与强迫症相关联。其中2个SNP还可预测人脑组织中的表达水平,1个SNP在报告基因研究中具有进一步的功能。在经过多重检验校正后,位于rs3087879、rs301430和rs7858819这3个SNP处的2个单倍型与强迫症显著相关,且包含2个与表达水平相关的SNP。此外,另一个与SLC1A1基因表达相关的SNP rs3933331,与强迫症囤积亚型相关,这是通过2个独立的、经过验证的量表评估得出的。
结论
我们的病例对照数据证实了先前规模较小的基于家系的研究,即SLC1A1是强迫症的一个易感基因座。我们使用的表达和基因型数据库挖掘方法为加强未来神经精神疾病及其他疾病的候选基因研究提供了一种潜在有用的补充方法。
Zotero 插件