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Considering Proximal Urea Cycle Disorders in Expanded Newborn Screening

机译:考虑近端尿素周期疾病在扩展新生儿筛查中

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摘要

Proximal urea cycle disorders (PUCDs) have adverse outcomes such as intellectual disability and death, which may benefit from newborn screening (NBS) through early detection and prevention with early treatment. Ornithine transcarbamylase deficiency (OTCD) and carbamoyl phosphate synthetase 1 deficiency (CPS1D) are screened in six and eight states in the United States. We analyzed current evidence to see if it supports inclusion of PUCDs in the NBS panels based upon prevention potential, medical, diagnostic, treatment, and public health rationales. A literature review was performed in PubMed using MESH terms for OTCD, CPS1D, and NAGSD. A systematic review was performed in the hallmark of NBS inclusion criteria. We reviewed 31 articles. Molecular and biochemical diagnosis is available to provide diagnostic evidence. Untreated PUCDs have a significant burden with considerable developmental delay and mortality that may improve with early treatment. Tandem mass spectrometry can be used for NBS for PUCDs; however, citrulline and glutamine alone are not specific. Medical treatments currently available for PUCDs meet existing medical, diagnostic, treatment, and public health rationales. Improvement in NBS algorithms to increase sensitivity and specificity will allow earlier diagnosis and treatment to potentially improve disability and mortality rates.
机译:近端尿素周期疾病(PUCD)具有不良结果,如智力残疾和死亡,这可能通过早期检测和预防新生儿筛查(NBS)受益于早期治疗。鸟氨酸转琥珀酰胺缺乏(OTCD)和氨基甲酰磷酸合成酶1缺乏(CPS1D)在美国的六个和八个州筛选。我们分析了当前证据,了解它是否支持基于预防潜在,医疗,诊断,治疗和公共卫生理由在国家统计局面板中纳入PUCD。使用网格术语为OTCD,CPS1D和NAGSD进行了文献综述。在NBS包含标准的标志中进行了系统审查。我们审查了31篇文章。分子和生物化学诊断可提供诊断证据。未经治疗的PUCD具有显着的负担,具有可能改善早期治疗的显着延迟和死亡率。串联质谱可用于PUCD的NBS;然而,单独的瓜氨酸和谷氨酰胺不具体。目前可用于PUCD的医疗治疗符合现有的医疗,诊断,治疗和公共卫生理由。 NBS算法的改进以提高敏感性和特异性,旨在提前诊断和治疗,以潜在地提高残疾和死亡率。

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