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Normal reference ranges for urinary δ‐aminolevulinic acid and porphobilinogen levels

机译:尿液δ-氨基乙酰酸和卟啉区的正常参考范围

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摘要

Acute hepatic porphyria (AHP) is a family of rare, serious, and potentially life‐threatening metabolic disorders caused by mutations in genes encoding enzymes involved in hepatic heme biosynthesis. AHP is characterized by accumulation of neurotoxic heme intermediates, δ‐aminolevulinic acid (ALA), and porphobilinogen (PBG), which are thought to be causal for the disease manifestations. Novel therapeutic treatments such as givosiran, an RNA interference therapeutic that was recently approved for treatment of adults with AHP, are focused on reducing the levels of ALA and PBG in patients toward levels observed in a healthy population. While there are two published reports on the distribution of urinary ALA and PBG levels in healthy subjects, these lacked the required details to enable the calculation of reference limits for ALA and PBG. Therefore, urinary ALA and PBG levels were quantified in 150 healthy subjects using a validated liquid chromatography tandem mass spectrometry (LC‐MS/MS) method that is highly sensitive, specific, accurate, and reproducible. These data were used to establish the upper limit of normal (ULN) values for ALA and PBG as 1.47 and 0.137 mmol/mol Cr, respectively. Relative to these ULN values, baseline urinary ALA and PBG levels in AHP patients were found to be 9.3‐ to 12‐fold, and 238‐ to 336‐fold higher, respectively. Results from this study can serve as a guide to assess the effectiveness of therapeutic interventions in lowering ALA and PBG.
机译:急性肝卟啉(AHP)是由肝血红素生物合成中的酶的突变引起的罕见,严重和威胁危及危及生命的代谢障碍。 AHP的特征在于神经毒性血红素中间体,δ-氨基乙酰丙烯酸(ALA)和卟啉硅(PBG)的积累,被认为是疾病表现的因果。新的治疗方法如Givosiran,最近批准用于治疗AHP的成人的RNA干扰治疗剂,重点是降低患者对健康人群观察到的水平的ALA和PBG水平。虽然有两份关于健康受试者的尿ALA和PBG水平分布的发表报告,但这些报告缺乏所需细节,以便计算ALA和PBG的参考限制。因此,使用验证的液相色谱串联质谱(LC-MS / MS)方法在150个健康受试者中量化尿ALA和PBG水平,该质谱法是高度敏感的,具体,准确和可重复的。这些数据用于分别建立ALA和PBG的正常(ULN)值的上限,分别为1.47和0.137mmol / mol CR。相对于这些ULN值,AHP患者的基线尿ALA和PBG水平分别为9.3至12倍,分别为238至336倍。本研究的结果可以作为评估降低ALA和PBG治疗干预措施的有效性的指南。

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