局灶性癫痫中已确立的癫痫基因中的新型变异。
Novel variants in established epilepsy genes in focal epilepsy.
机构信息
Neurology Clinic, University Clinical Center of Serbia, Belgrade, Serbia; Faculty of Medicine, University of Belgrade, Belgrade, Serbia.
Faculty of Medicine, University of Belgrade, Belgrade, Serbia.
出版信息
Seizure. 2023 Aug;110:146-152. doi: 10.1016/j.seizure.2023.06.005. Epub 2023 Jun 7.
INTRODUCTION
Next generation sequencing (NGS) has greatly expanded our understanding of genetic contributors in multiple epilepsy syndromes, including focal epilepsy. Describing the genetic architecture of common syndromes promises to facilitate the diagnostic process as well as aid in the identification of patients who stand to benefit from genetic testing, but most studies to date have been limited to examining children or adults with intellectual disability. Our aim was to determine the yield of targeted sequencing of 5 established epilepsy genes (DEPDC5, LGI1, SCN1A, GRIN2A, and PCHD19) in an extensively phenotyped cohort of focal epilepsy patients with normal intellectual function or mild intellectual disability, as well as describe novel variants and determine the characteristics of variant carriers.
PATIENTS AND METHODS
Targeted panel sequencing was performed on 96 patients with a strong clinical suspicion of genetic focal epilepsy. Patients had previously gone through a comprehensive diagnostic epilepsy evaluation in The Neurology Clinic, University Clinical Center of Serbia. Variants of interest (VOI) were classified using the American College of Medical Genetics and the Association for Molecular Pathology criteria.
RESULTS
Six VOI in eight (8/96, 8.3%) patients were found in our cohort. Four likely pathogenic VOI were determined in six (6/96, 6.2%) patients, two DEPDC5 variants in two patients, one SCN1A variant in two patients and one PCDH19 variant in two patients. One variant of unknown significance (VUS) was found in GRIN2A in one (1/96, 1.0%) patient. Only one VOI in GRIN2A was classified as likely benign. No VOI were detected in LGI1.
CONCLUSION
Sequencing of only five known epilepsy genes yielded a diagnostic result in 6.2% of our cohort and revealed multiple novel variants. Further research is necessary for a better understanding of the genetic basis in common epilepsy syndromes in patients with normal intellectual function or mild intellectual disability.
简介
下一代测序(NGS)极大地扩展了我们对多种癫痫综合征(包括局灶性癫痫)中遗传因素的理解。描述常见综合征的遗传结构有望促进诊断过程,并有助于确定受益于基因检测的患者,但迄今为止的大多数研究都仅限于检查智力障碍的儿童或成人。我们的目的是确定在具有正常智力或轻度智力障碍的局灶性癫痫患者中,对 5 种已建立的癫痫基因(DEPDC5、LGI1、SCN1A、GRIN2A 和 PCHD19)进行靶向测序的效果,描述新的变异体,并确定变异体携带者的特征。
患者和方法
对 96 例具有强烈遗传局灶性癫痫临床怀疑的患者进行了靶向panel 测序。这些患者之前已经在塞尔维亚大学临床中心神经病学诊所进行了全面的诊断性癫痫评估。使用美国医学遗传学学院和分子病理学协会的标准对感兴趣的变异(VOI)进行分类。
结果
在我们的队列中发现了 8 例(8/96,8.3%)患者中的 6 个 VOI。在 6 例(6/96,6.2%)患者中确定了 4 个可能致病性 VOI,其中 2 例患者存在 DEPDC5 变异,2 例患者存在 SCN1A 变异,2 例患者存在 PCDH19 变异。在 1 例(1/96,1.0%)患者的 GRIN2A 中发现了 1 个意义不明的变异(VUS)。仅在 GRIN2A 中发现了 1 个 VOI 被归类为可能良性。在 LGI1 中未检测到 VOI。
结论
仅对 5 个已知的癫痫基因进行测序,在我们的队列中产生了 6.2%的诊断结果,并揭示了多个新的变异体。需要进一步的研究来更好地了解智力正常或轻度智力障碍患者常见癫痫综合征的遗传基础。
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