Mei Daoqi, Gu Yu, Zhang Bingbing, Mei Shiyue, Wang Xiaona, Ma Yuanning, Deng Jie, Tang Jihong
Department of Neurology, Children's Hospital Affiliated to Suzhou University, No. 92, Zhong Nan Street, Suzhou Industrial Park, Suzhou, 215025, Jiangsu Province, China.
Department of Pediatrics, Children's Hospital Affiliated to Zhengzhou University, Henan Children's Hospital, Zhengzhou Children's Hospital, 33 Longhu Waihuan East Road, Jinshui District, Zhengzhou, 450018, Henan ProvinceChina, China.
Orphanet J Rare Dis. 2025 Aug 18;20(1):440. doi: 10.1186/s13023-025-03984-x.
To summarize the clinical characteristics of a cohort of nine Chinese children with GNAO1 encephalopathy and analyze their genotypes.
A retrospective study was conducted on nine children diagnosed with GNAO1 encephalopathy at the Neurology Department of two children's hospitals between January 2019 and December 2022. Their clinical manifestations, genetic test results, cranial imaging, electroencephalography and treatment were summarized. Their prognosis was followed up.
All nine patients presented with moderate-to-severe psychomotor developmental delay and dystonia. Six patients exhibited neonatal or infantile-onset epilepsy, manifesting as generalized tonic-clonic seizure, myoclonic seizure, epileptic spasms, and were diagnosed with developmental and epileptic encephalopathy 17 (DEE 17). Two patients presented with choreoathetosis in infancy without epileptic seizure and were diagnosed with the neurodevelopmental disorder with involuntary movements (NEDIM). One patient presented with choreoathetosis at two years of age and developed focal seizures at six years of age, representing an intermediate phenotype. During a follow-up period of 0.8-3.5 years, one child died due to infection. The remaining eight continued to exhibit psychomotor retardation. Pathogenic or likely pathogenic de novo heterozygous missense variants in GNAO1 were identified in all nine cases. Among these, the variants c.17G > T (p.Ser6Ile), c.119G > C (p.Gly40Ala), and c.748 C > T (p.Leu250Phe) are novel.
In conclusion, we analyzed the clinical characteristics and genetic variants of a cohort of nine Chinese children with GNAO1 variants and identified three novel GNAO1 variants. Our study expanded the spectrum of genotypes and phenotypes in GNOA1-associated encephalopathy.
总结9例中国儿童GNAO1脑病患者的临床特征并分析其基因型。
对2019年1月至2022年12月期间在两家儿童医院神经科确诊为GNAO1脑病的9例儿童进行回顾性研究。总结他们的临床表现、基因检测结果、头颅影像学、脑电图及治疗情况。对其预后进行随访。
9例患者均有中重度精神运动发育迟缓及肌张力障碍。6例患者有新生儿期或婴儿期起病的癫痫,表现为全身强直阵挛发作、肌阵挛发作、癫痫性痉挛,被诊断为发育性癫痫性脑病17型(DEE 17)。2例患者婴儿期出现舞蹈手足徐动症,无癫痫发作,被诊断为伴有不自主运动的神经发育障碍(NEDIM)。1例患者2岁时出现舞蹈手足徐动症,6岁时出现局灶性癫痫发作,表现为中间型表型。在0.8至3.5年的随访期内,1例儿童因感染死亡。其余8例仍有精神运动发育迟缓。9例均鉴定出GNAO1基因致病性或可能致病性的新生杂合错义变异。其中,变异c.17G>T(p.Ser6Ile)、c.119G>C(p.Gly40Ala)和c.748C>T(p.Leu250Phe)为新发现变异。
总之,我们分析了9例携带GNAO1变异的中国儿童的临床特征和基因变异,鉴定出3个新的GNAO1变异。我们的研究扩展了GNOA1相关脑病的基因型和表型谱。
