调控遗传变异对RAI1基因表达水平的影响机制及其与孤独症的关系

项目名称： 调控遗传变异对RAI1基因表达水平的影响机制及其与孤独症的关系

项目编号： No.31200937

项目类型： 青年科学基金项目

立项/批准年度： 2013

项目学科： 遗传学与生物信息学、细胞生物学

项目作者： 陈莉

作者单位： 复旦大学

项目金额： 21万元

中文摘要： 视黄酸诱导基因1（RAI1）是染色体17p11.2不稳定区的剂量敏感基因，其缺失重复与多种精神疾病包括孤独症相关。该拷贝数变异对基因表达产物的剂量效应可以由调控遗传变异通过改变mRNA转录，剪切和稳定性进而改变基因表达水平来模拟，所以RAI1的调控遗传变异可能与散发孤独症不同症状程度有关。前期实验发现RAI1在人脑等位基因表达不平衡，脑表达量和基因型关联分析及群体分布数学模型提示存在两个调节RAI1表达的遗传变异。本课题拟通过凝胶迁移、染色质免疫沉淀、不同等位基因荧光素酶报告载体和第二代测序等手段，研究RAI1调控遗传变异作用机制，并应用到孤独症病例对照关联研究中，探索RAI1剂量效应与孤独症不同症状程度的关系。本研究创新性的将调控遗传变异及组合作为研究孤独症复杂症状的切入点，结合群体分布数学模型和第二代测序AEI基因型比对方法，为病例对照关联分析提供更具生物学意义和操作可行性的分子标记。

中文关键词： 视黄酸诱导基因 1（RAI1）；表达数量性状位点；孤独症；视黄酸受体结合位点；DEAF1自调节转录因子

英文摘要： Retinoic acid induced-1 (RAI1) is a dose-sensitive gene located at Ch17p11.2, an unstable region that occasionally undergoes deletion or duplication during meiosis. Deletions at this locus cause Smith-Magenis syndrome (SMS) and duplications cause Potocki-Lupski syndrome (PTLS), complex developmental disorders that include autistic behaviors among their symptoms. Recent studies have identified RAI1 as the key gene in both disorders, suggesting that changes in RAI1 copy number may be a cause of autism. Because regulatory genetic variants, which influence gene expression by modulating mRNA transcription, splicing, or mRNA stability, can mimic the effects gene deletions or duplications, we hypothesize that common regulatory variants of RAI1 may contribute to sporadic autism. In the preliminary experiments, we used a novel next-generation DNA sequencing assay for allelic expression imbalance (AEI), quantitative PCR assays and mathematical modeling of population distribution to show that mRNA expression of RAI1 in human prefrontal cortex is regulated by two regulatory variants, at least one of which is located in the extended 5'-region of the gene. In this study, we propose to use electrophoretic mobility shift, chromatin immunoprecipitation and luciferase reporter assays in combination with next-generation DNA sequen

英文关键词： RAI1 (retinoic acid induced-1)；expression Quantitative Trait Loci;（eQTLs）；autism；retinoic acid RXR-RAR receptors；DEAF1 (Deformed epidermal autoregulatory factor-1)