Naseer Muhammad Imran, Faheem Muhammad, Chaudhary Adeel G, Kumosani Taha A, Al-Quaiti Maha Mohsin, Jan Mohammed M, Saleh Jamal Hasan, Al-Qahtani Mohammad H
BMC Genomics. 2015;16 Suppl 1(Suppl 1):S10. doi: 10.1186/1471-2164-16-S1-S10. Epub 2015 Jan 15.
Epilepsy is genetically complex neurological disorder affecting millions of people of different age groups varying in its type and severity. Copy number variants (CNVs) are key players in the genetic etiology of numerous neurodevelopmental disorders and prior findings also revealed that chromosomal aberrations are more susceptible against the pathogenesis of epilepsy. Novel technologies, such as array comparative genomic hybridization (array-CGH), may help to uncover the pathogenic CNVs in patients with epilepsy.
This study was carried out by high density whole genome array-CGH analysis with blood DNA samples from a cohort of 22 epilepsy patients to search for CNVs associated with epilepsy. Pathogenic rearrangements which include 6p12.1 microduplications in 5 patients covering a total region of 99.9kb and 7q32.3 microdeletions in 3 patients covering a total region of 63.9kb were detected. Two genes BMP5 and PODXL were located in the predicted duplicated and deleted regions respectively. Furthermore, these CNV findings were confirmed by qPCR.
We have described, for the first time, several novel CNVs/genes implicated in epilepsy in the Saudi population. These findings enable us to better describe the genetic variations in epilepsy, and could provide a foundation for understanding the critical regions of the genome which might be involved in the development of epilepsy.
癫痫是一种具有遗传复杂性的神经系统疾病,影响着数百万不同年龄组的人群,其类型和严重程度各不相同。拷贝数变异(CNV)是众多神经发育障碍遗传病因中的关键因素,先前的研究结果还表明,染色体畸变更容易引发癫痫的发病机制。诸如阵列比较基因组杂交(array-CGH)等新技术可能有助于发现癫痫患者中的致病性CNV。
本研究通过对22例癫痫患者队列的血液DNA样本进行高密度全基因组array-CGH分析,以寻找与癫痫相关的CNV。检测到致病性重排,其中包括5例患者的6p12.1微重复,总区域为99.9kb,以及3例患者的7q32.3微缺失,总区域为63.9kb。两个基因BMP5和PODXL分别位于预测的重复和缺失区域。此外,这些CNV结果通过qPCR得到了证实。
我们首次描述了沙特人群中与癫痫相关的几种新型CNV/基因。这些发现使我们能够更好地描述癫痫中的遗传变异,并可为理解可能参与癫痫发生发展的基因组关键区域提供基础。
