Nguyen Thi Thanh Ngan, Khanh Nguyen Ngoc, Vu Chi Dung, Nguyen Ngoc-Lan, Tran Van Khanh, Lien Nguyen Thi Kim, Van Tung Nguyen, Quan Nguyen Duc, Hien Nguyen Thanh, Giang Tran Thi Huong, Xuan Nguyen Thi, Tao Nguyen Thien, Khoa Tran Van, Nguyen Huy Hoang
Institute of Genome Research, Vietnam Academy of Science and Technology (VAST), Hanoi, Vietnam.
Center of Endocrinology, Metabolism, Genetic/Genomics and Molecular Therapy, Vietnam National Children's Hospital, Hanoi, Vietnam.
Front Pediatr. 2024 Dec 10;12:1494604. doi: 10.3389/fped.2024.1494604. eCollection 2024.
A pyruvate dehydrogenase complex deficiency causes a reduction in adenosine triphosphate production and energy insufficiency, leading to neurological disorders. An abnormal E1-alpha protein originating from the gene with pathogenic variants is unable to communicate with E1-beta for the formation of the E1 enzyme, decreasing pyruvate dehydrogenase complex activity. In this study, we report a Vietnamese boy with lethargy, severe metabolic acidosis, increased serum lactate, hyperalaninemia, lactic acidosis, and globus pallidus lesions. Whole-exome sequencing and variant filtering identified a hemizygous missense variant NM000284.4 (): c.479T>G (p.Phe160Cys) in the patient. The variant c.479T>G caused a single nucleotide substitution on exon 5 and was predicted to be a disease-causing variant in the analyses. We present the first report with a genetic analysis of a Vietnamese patient with pyruvate dehydrogenase E1-alpha deficiency (PDHAD). Sanger sequencing demonstrated that the patient inherited the variant from his mother who harbored the variant in a heterozygous state, but no PDHAD symptoms were observed in her. In addition, a prenatal test of the patient's mother revealed a fetus with a normal genotype. Furthermore, the patient's father and sister both carried a normal allele. Based on the American College of Medical Genetics criteria, the variant c.479T>G was predicted to be a likely pathogenic variant. Using the combination of the patient's genotype and phenotype, he was definitively diagnosed with pyruvate dehydrogenase E1-alpha deficiency. Our findings expand the mutational spectrum of neurological disorders and provide the scientific basis for genetic counseling for the patient's family.
丙酮酸脱氢酶复合物缺乏症会导致三磷酸腺苷生成减少和能量不足,进而引发神经障碍。源自具有致病性变异基因的异常E1-α蛋白无法与E1-β相互作用形成E1酶,从而降低丙酮酸脱氢酶复合物的活性。在本研究中,我们报告了一名患有嗜睡、严重代谢性酸中毒、血清乳酸升高、高丙氨酸血症、乳酸性酸中毒和苍白球病变的越南男孩。全外显子组测序和变异筛选在该患者中鉴定出一个半合子错义变异NM000284.4():c.479T>G(p.Phe160Cys)。变异c.479T>G在外显子5上引起单核苷酸替换,在分析中被预测为致病变异。我们首次报告了对一名患有丙酮酸脱氢酶E1-α缺乏症(PDHAD)的越南患者的基因分析。桑格测序表明,患者从其母亲那里遗传了该变异,其母亲为该变异的杂合携带者,但未观察到她有PDHAD症状。此外,对患者母亲的产前检测显示胎儿基因型正常。此外,患者的父亲和姐姐均携带正常等位基因。根据美国医学遗传学学会的标准,变异c.479T>G被预测为可能的致病变异。结合患者的基因型和表型,他被明确诊断为丙酮酸脱氢酶E1-α缺乏症。我们的研究结果扩展了神经障碍的突变谱,并为患者家庭的遗传咨询提供了科学依据。
