先天性生酮错误：四名患者的新变异、临床表现和随访。

IF 0.8 4区社会学 Q3 SOCIOLOGY

Zeitschrift Fur Soziologie Pub Date : 2022-07-12 eCollection Date: 2024-03-01 DOI:10.1055/s-0042-1749362

Haseena Sait, Somya Srivastava, Somesh Kumar, Bijo Varughese, Manmohan Pandey, Manjunath Venkatramaiah, Parul Chaudhary, Amita Moirangthem, Kausik Mandal, Seema Kapoor

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引用次数: 0

摘要

先天性生酮错误是一种罕见的疾病，会在脂肪分解应激时导致急性和暴发性失代偿，尤其是在婴儿和儿童中。这些疾病包括线粒体 3-羟基-3-甲基戊二酰-CoA（HMG-CoA）合成酶（HMGCS）缺乏症和 HMG-CoA 裂解酶（HMGCL）缺乏症。在这个系列中，我们描述了四名患者的临床、生化和分子特征，以及饮食干预和长期随访的结果。我们对 HMGCS 和 HMGCL 缺乏症患者各两名进行了临床病史评估和生化检查，包括串联质谱法（TMS）和尿液气相色谱-质谱法（GCMS）。分子分析是通过全外显子组测序以及长程聚合酶链反应验证的外显子阵列进行的。除一名 HMGCL 缺乏症患者在 5 岁时首次发病外，所有患者均在婴儿期早期被诊断为急性代谢失调。所有患者都出现了中枢神经系统表现、严重的代谢性酸中毒、高氨血症、低血糖但乳酸正常以及尿酮体缺失。其中三人的病情危及生命，一人因病死亡。TMS 为非特异性，尿液 GCMS 显示 HMGCS 缺乏症患者有二羧酸尿症。两名 HMGCL 缺乏症患者的 TMS 和尿液 GCMS 均显示 3-羟基异戊酰基肉碱水平升高，尿液 GCMS 则显示亮氨酸降解代谢物升高。我们发现了五个新型变异体，其中包括涉及 HMGCL 基因第 2 外显子的大缺失。没有证据表明在世的个体会出现长期的神经系统后遗症。两名 HMGCS 缺乏症患者在饮食中摄入适量脂肪。HMGCL 缺乏症患者的饮食则以低亮氨酸和蛋白质为主，适量摄入脂肪。所有患者均恢复良好，没有再出现新陈代谢失调的情况。

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Inborn Errors of Ketogenesis: Novel Variants, Clinical Presentation, and Follow-Up in a Series of Four Patients.

Inborn errors of ketogenesis are rare disorders that result in acute and fulminant decompensation during lipolytic stress, particularly in infants and children. These include mitochondrial 3-hydroxy-3-methylglutaryl-CoA (HMG-CoA) synthase (HMGCS) deficiency and HMG-CoA lyase (HMGCL) deficiency. In this series, we describe the clinical, biochemical, and molecular profiles of four patients along with dietary interventions and their outcomes on a long-term follow-up. Two patients each of HMGCS and HMGCL deficiency were evaluated with clinical history, biochemical investigations, including tandem mass spectrometry (TMS) and urine gas chromatography-mass spectrometry (GCMS). Molecular analysis was performed by whole-exome sequencing, as well as exon array validated by long-range polymerase chain reaction. All individuals were diagnosed with acute metabolic decompensation in the early infancy period except one with HMGCL deficiency who had the first presentation at 5 years of age. Central nervous system manifestations, severe metabolic acidosis, hyperammonemia, hypoglycemia with a normal lactate, and absence of urinary ketones were observed in all the affected individuals. The disorder was life-threatening in three individuals and one succumbed to the illness. TMS was nonspecific and urine GCMS revealed dicarboxylic aciduria in HMGCS deficiency. Both the patients with HMGCL deficiency demonstrated elevated 3 hydroxyisovaleryl carnitine levels in TMS and metabolites of leucine degradation in urine GCMS. We identified five novel variants that included a large deletion involving exon 2 in HMGCL gene. There was no evidence of long-term neurological sequelae in the living individuals. Diet with moderation of fat intake was followed in two individuals with HMGCS deficiency. Low leucine and protein diet with moderation of fat intake was followed in the individual with HMGCL deficiency. All affected individuals are thriving well with no further major metabolic decompensation.

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来源期刊

Zeitschrift Fur Soziologie SOCIOLOGY-

CiteScore

1.30

自引率

12.50%

发文量

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