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Aspects of Newborn Screening in Isovaleric Acidemia

机译:新生儿筛选在异戊酸血症方面

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摘要

Isovaleric acidemia (IVA), an inborn error of leucine catabolism, is caused by mutations in the isovaleryl-CoA dehydrogenase (IVD) gene, resulting in the accumulation of derivatives of isovaleryl-CoA including isovaleryl (C5)-carnitine, the marker metabolite used for newborn screening (NBS). The inclusion of IVA in NBS programs in many countries has broadened knowledge of the variability of the condition, whereas prior to NBS, two distinct clinical phenotypes were known, an “acute neonatal” and a “chronic intermittent” form. An additional biochemically mild and potentially asymptomatic form of IVA and its association with a common missense mutation, c.932C>T (p.A282V), was discovered in subjects identified through NBS. Deficiency of short/branched chain specific acyl-CoA dehydrogenase (2-methylbutyryl-CoA dehydrogenase), a defect of isoleucine degradation whose clinical significance remains unclear, also results in elevated C5-carnitine, and may therefore be detected by NBS for IVA. Treatment strategies for the long-term management of symptomatic IVA comprise the prevention of catabolism, dietary restriction of natural protein or leucine intake, and supplementation with l-carnitine and/or l-glycine. Recommendations on how to counsel and manage individuals with the mild phenotype detected by NBS are required.
机译:异戊酸酸亚酸血症(IVA),亮氨酸脱蛋白的原始误差是由异戊糖-CoA脱氢酶(IVD)基因的突变引起的,导致脱象衍生物的衍生物的累积,包括异戊烯烃(C5)-Carnitine,所使用的标志物代谢物对于新生儿筛查(NBS)。在许多国家的NBS方案中包含IVA在NBS方案中扩大了对病症的可变性的了解,而在NBS之前,已知两个不同的临床表型,是“急性新生儿”和“慢性间歇性”形式。在通过NB鉴定的受试者中发现了额外的生物化学上和其与常见的畸形突变和其与常见的畸形突变相关性C.932C> T(P.A282V)的关系。短/支链特异性酰基-CoA脱氢酶(2-甲基丁酰基-CoA脱氢酶)的缺乏,其临床意义仍不清楚的异亮氨酸降解的缺陷,也导致升高的C5肉碱,因此可以通过NBS对IVA检测。对症状IVA的长期管理的治疗策略包括预防分解代谢,天然蛋白质或亮氨酸摄入的膳食限制,并用L-肉碱和/或L-甘氨酸补充。关于如何律师和管理NBS检测到的轻度表型的个人的建议。

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