TSEN54 Gene-Related Pontocerebellar Hypoplasia Type 2 in a Newborn with Refractory Myoclonic Seizures

Q4 Medicine

Annals of Child Neurology Pub Date : 2022-06-28 DOI:10.26815/acn.2022.00178

J. Byun, J. Ha, C. Kim

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Abstract

Neonates are vulnerable to epileptic seizures. Eighty percent of neonatal seizures occur in the first 1 or 2 days of life. The most common cause of neonatal seizures is hypoxic ischemic encephalopathy. Brain malformations can also be an important cause of seizures. Herein, we present a case of an infant who experienced severe myoclonic seizures with little response to anti-seizure medications from the first day of life. The infant had refractory myoclonic seizures associated with pontocerebellar hypoplasia (PCH) and a mutation in transfer ribonucleic acid splicing endonuclease 54 (TSEN54). This case was reviewed and approved by the Institutional Review Board of Keimyung University Dongsan Hospital (IRB No. 2022-04-017). The requirement for informed consent was waived by the board. A female infant was born at 38 weeks of gestation by cesarean section due to breech presentation at a local hospital. She had a birth weight of 2,840 g (25th to 50th percentile), length of 45 cm (10th to 25th percentile), and head circumference of 31 cm ( < 10th percentile). Although her Apgar scores were 7 and 9 at 1 and 5 minutes, respectively, the baby suffered from severe seizures and respiratory distress from the first day of life. Therefore, she was transferred to a university hospital. A neurological examination revealed generalized myoclonic seizures with respiratory distress, hypertonia of the extremities, joint stiffness of both elbows, and increased deep tendon reflexes. Initial electroencephalography (EEG) showed frequent ictal EEG patterns with 6 to 7 Hz rhythmic activities beginning at P3, P4, and T6 independently. Radiologic studies (Fig. 1) showed a flat ventral pons and a small cerebellum. This baby had no specific findings in studies for metabolic disorders or genetic screening tests associated with early myoclonic seizures in infancy. To determine the genetic cause of PCH, targeted exome sequencing was performed when she was 1 month of age. Finally, two variants of the TSEN54 gene, c.919G > T and c. 623G > A, were found, representing compound heterozygosity. These two variants were confirmed by Sanger sequencing (Fig. 2), and no other copy number variation was found in the diagnostic exome sequencing study. The c.919G > T mutation (NM_ 207346.2:c.919G > T, p.Ala307Ser, rs1139941 52) has been already reported as the most common TSEN54 variant found in PCH patients [1,2], and has been classified as a pathogenic variant in the ClinVar database. It is very rare in large population databases, such as gnomAD (https:// gnomad.broadinstitute.org/), where it has a minor allele frequency (MAF) of 0.09%, and KorepISSN 2635-909X • eISSN 2635-9103 Ann Child Neurol 2022;30(3):152-154 https://doi.org/10.26815/acn.2022.00178

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TSEN54基因相关的2型桥小脑发育不全新生儿难治性肌阵挛性发作

新生儿易患癫痫发作。80%的新生儿癫痫发作发生在出生后的1到2天。新生儿癫痫发作最常见的原因是缺氧缺血性脑病。大脑畸形也是癫痫发作的重要原因。在这里，我们提出了一个婴儿谁经历了严重的肌阵挛性癫痫发作，从生命的第一天起，对抗癫痫药物的反应很小。婴儿患有顽固性肌阵挛性发作，伴有桥小脑发育不全(PCH)和转移核糖核酸剪接内切酶54 (TSEN54)突变。本病例由启明大学东山医院机构审查委员会(IRB No. 2022-04-017)审查并批准。董事会放弃了知情同意的要求。一名女婴儿在妊娠38周时在当地医院因臀位出现剖宫产。出生体重2840 g(25 - 50百分位)，体长45 cm(10 - 25百分位)，头围31 cm(< 10百分位)。虽然她的阿普加评分在1分钟和5分钟时分别为7分和9分，但婴儿从出生的第一天起就患有严重的癫痫发作和呼吸窘迫。因此，她被转到大学医院。神经学检查显示全身性肌阵挛性发作伴呼吸窘迫，四肢张力增高，双肘关节僵硬，深腱反射增加。初始脑电图(EEG)显示频繁的节律性脑电图模式，分别在P3, P4和T6开始6至7 Hz的节律性活动。放射学检查(图1)显示平坦的腹侧脑桥和小的小脑。该婴儿在与婴儿期早期肌阵挛性发作相关的代谢紊乱或基因筛查试验研究中没有具体发现。为了确定PCH的遗传原因，在她1个月大时进行了靶向外显子组测序。最后，发现TSEN54基因的c. 919g > T和c. 623G > A两个变体，表现为复合杂合性。Sanger测序证实了这两个变异(图2)，在诊断外显子组测序研究中未发现其他拷贝数变异。c. 919g . > T突变(NM_ 207346.2:c。919G > T, p.a ala307ser, rs1139941 52)已被报道为PCH患者中最常见的TSEN54变异[1,2]，并在ClinVar数据库中被归类为致病性变异。在大型人口数据库中非常罕见，例如gnomAD (https:// gnomad.broadinstitute.org/)，)，其次要等位基因频率(MAF)为0.09%，KorepISSN 2635-909X•eISSN 2635-9103 Ann Child Neurol 2022;30(3):152-154 https://doi.org/10.26815/acn.2022.00178

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来源期刊

Annals of Child Neurology Medicine-Pediatrics, Perinatology and Child Health

CiteScore

0.50

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0.00%

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审稿时长

8 weeks