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用于监测苯丙酮尿症患者的血液苯丙氨酸测量实验室检测的性能。

Performance of laboratory tests used to measure blood phenylalanine for the monitoring of patients with phenylketonuria.

作者信息

Moat Stuart J, Schulenburg-Brand Danja, Lemonde Hugh, Bonham James R, Weykamp Cas W, Mei Joanne V, Shortland Graham S, Carling Rachel S

机构信息

Department of Medical Biochemistry, Immunology & Toxicology, University Hospital Wales, Cardiff, UK.

School of Medicine, Cardiff University, University Hospital Wales, Cardiff, UK.

出版信息

J Inherit Metab Dis. 2020 Mar;43(2):179-188. doi: 10.1002/jimd.12163. Epub 2019 Oct 2.

Abstract

Analysis of blood phenylalanine is central to the monitoring of patients with phenylketonuria (PKU) and age-related phenylalanine target treatment-ranges (0-12 years; 120-360 μmol/L, and >12 years; 120-600 μmol/L) are recommended in order to prevent adverse neurological outcomes. These target treatment-ranges are based upon plasma phenylalanine concentrations. However, patients are routinely monitored using dried bloodspot (DBS) specimens due to the convenience of collection. Significant differences exist between phenylalanine concentrations in plasma and DBS, with phenylalanine concentrations in DBS specimens analyzed by flow-injection analysis tandem mass spectrometry reported to be 18% to 28% lower than paired plasma concentrations analyzed using ion-exchange chromatography. DBS specimens with phenylalanine concentrations of 360 and 600 μmol/L, at the critical upper-target treatment-range thresholds would be plasma equivalents of 461 and 768 μmol/L, respectively, when a reported difference of 28% is taken into account. Furthermore, analytical test imprecision and bias in conjunction with pre-analytical factors such as volume and quality of blood applied to filter paper collection devices to produce DBS specimens affect the final test results. Reporting of inaccurate patient results when comparing DBS results to target treatment-ranges based on plasma concentrations, together with inter-laboratory imprecision could have a significant impact on patient management resulting in inappropriate dietary change and potentially adverse patient outcomes. This review is intended to provide perspective on the issues related to the measurement of phenylalanine in blood specimens and to provide direction for the future needs of PKU patients to ensure reliable monitoring of metabolic control using the target treatment-ranges.

摘要

血液苯丙氨酸分析是苯丙酮尿症(PKU)患者监测的核心,为预防不良神经学后果,推荐了与年龄相关的苯丙氨酸目标治疗范围(0 - 12岁;120 - 360μmol/L,以及>12岁;120 - 600μmol/L)。这些目标治疗范围基于血浆苯丙氨酸浓度。然而,由于采集方便,患者通常使用干血斑(DBS)标本进行监测。血浆和DBS中的苯丙氨酸浓度存在显著差异,据报道,采用流动注射分析串联质谱法分析的DBS标本中的苯丙氨酸浓度比使用离子交换色谱法分析的配对血浆浓度低18%至28%。当考虑到报告的28%的差异时,苯丙氨酸浓度分别为360和600μmol/L的DBS标本,在临界目标治疗范围上限阈值时,其血浆等效浓度分别为461和768μmol/L。此外,分析测试的不精密度和偏差,连同诸如应用于滤纸采集装置以产生DBS标本的血液体积和质量等分析前因素,都会影响最终测试结果。将DBS结果与基于血浆浓度的目标治疗范围进行比较时报告不准确的患者结果,以及实验室间的不精密度,可能会对患者管理产生重大影响,导致不适当的饮食改变和潜在的不良患者结局。本综述旨在阐述与血液标本中苯丙氨酸测量相关的问题,并为PKU患者的未来需求提供方向,以确保使用目标治疗范围可靠地监测代谢控制情况。

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