Department of Genetics, Yale University, 464 Congress Avenue, Suite 243, New Haven, CT 06520, USA.
Am J Hum Genet. 2013 Jul 11;93(1):19-28. doi: 10.1016/j.ajhg.2013.05.008. Epub 2013 Jun 6.
Reading disability (RD) and language impairment (LI) are common learning disabilities that make acquisition and utilization of reading and verbal language skills, respectively, difficult for affected individuals. Both disorders have a substantial genetic component with complex inheritance. Despite decades of study, reading and language, like many other complex traits, consistently evade identification of causative and functional variants. We previously identified a putative functional risk variant, named BV677278 for its GenBank accession number, for RD in DCDC2. This variant consists of an intronic microdeletion and a highly polymorphic short tandem repeat (STR) within its breakpoints. We have also shown this STR to bind to an unknown nuclear protein with high specificity. Here, we replicate BV677278's association with RD, expand its association to LI, identify the BV677278-binding protein as the transcription factor ETV6, and provide compelling genetic evidence that BV677278 is a regulatory element that influences reading and language skills. We also provide evidence that BV677278 interacts nonadditively with KIAA0319, an RD-associated gene, to adversely affect several reading and cognitive phenotypes. On the basis of these data, we propose a new name for BV677278: "READ1" or "regulatory element associated with dyslexia 1."
阅读障碍 (RD) 和语言障碍 (LI) 是常见的学习障碍,分别使受影响的个体难以获得和运用阅读和口头语言技能。这两种疾病都有很大的遗传成分,具有复杂的遗传。尽管经过几十年的研究,阅读和语言,就像许多其他复杂特征一样,仍然无法确定其致病和功能变体。我们之前在 DCDC2 中发现了一个名为 BV677278 的假定功能风险变体,它的 GenBank 登录号为其命名。该变体由内含子微缺失和其断点内的高度多态性短串联重复 (STR) 组成。我们还表明,这种 STR 与一种未知的核蛋白具有高度特异性结合。在这里,我们复制了 BV677278 与 RD 的关联,将其与 LI 的关联扩展,确定 BV677278 结合蛋白为转录因子 ETV6,并提供了令人信服的遗传证据,证明 BV677278 是一个调节元件,影响阅读和语言技能。我们还提供了证据表明,BV677278 与 RD 相关基因 KIAA0319 非加性相互作用,对几个阅读和认知表型产生不利影响。基于这些数据,我们提出了 BV677278 的新名称:“READ1”或“与阅读障碍相关的调节元件 1”。
