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雅培 Alinity c 分析系统上六种酶测量的可追溯性验证。

Traceability validation of six enzyme measurements on the Abbott Alinity c analytical system.

机构信息

Research Centre for Metrological Traceability in Laboratory Medicine (CIRME), University of Milan, Milan, Italy.

Department of Laboratory Medicine, Collegium Medicum, Nicolaus Copernicus University, Torun, Poland.

出版信息

Clin Chem Lab Med. 2020 Jul 28;58(8):1250-1256. doi: 10.1515/cclm-2020-0015.

Abstract

Background Laboratory professionals should independently verify the correct implementation of metrological traceability of commercial measuring systems and determine if their performance is fit for purpose. We evaluated the trueness, uncertainty of measurements, and transferability of six clinically important enzyme measurements (alanine aminotransferase [ALT], alkaline phosphatase [ALP], aspartate aminotransferase [AST], creatine kinase [CK], γ-glutamyltransferase [γGT], and lactate dehydrogenase [LDH]) performed on the Abbott Alinity c analytical system. Methods Target values and associated uncertainties were assigned to three pools for each enzyme by using the International Federation of Clinical Chemistry and Laboratory Medicine (IFCC) reference measurement procedures (RMPs) and the pools were then measured on the Alinity system. Bias estimation and regression studies were performed, and the uncertainty associated with Alinity measurements was also estimated, using analytical performance specifications (APS) derived from biological variability of measurands as goals. Finally, to validate the transferability of the obtained results, a comparison study between two Alinity systems located in Milan, Italy, and Bydgoszcz, Poland, was carried out. Results Correct implementation of traceability to the IFCC RMPs and acceptable measurement uncertainty fulfilling desirable (ALP, AST, LDH) or optimal APS (ALT, CK, γGT) was verified for all evaluated enzymes. An optimal alignment between the two Alinity systems located in Milan and Bydgoszcz was also found for all enzyme measurements. Conclusions We confirmed that measurements of ALT, ALP, AST, CK, γGT, and LDH performed on the Alinity c analytical system are correctly standardized to the IFCC reference measurement systems and the system alignment is consistent between different platforms.

摘要

背景 实验室专业人员应独立验证商业测量系统计量溯源的正确实施情况,并确定其性能是否符合预期用途。我们评估了 Abbott Alinity c 分析系统上进行的六种重要临床酶测量(丙氨酸氨基转移酶[ALT]、碱性磷酸酶[ALP]、天门冬氨酸氨基转移酶[AST]、肌酸激酶[CK]、γ-谷氨酰转移酶[γGT]和乳酸脱氢酶[LDH])的准确度、测量不确定度和可转移性。

方法 通过使用国际临床化学和实验室医学联合会(IFCC)参考测量程序(RMP)为每个酶的三个样本池赋值目标值及其相关不确定度,然后在 Alinity 系统上测量这些样本池。进行了偏差估计和回归研究,并使用基于测量物生物变异性的分析性能规格(APS)来估计与 Alinity 测量相关的不确定度,这些 APS 用作目标。最后,为了验证获得的结果的可转移性,在位于意大利米兰和波兰比得哥什的两个 Alinity 系统之间进行了比较研究。

结果 对于所有评估的酶,均验证了溯源至 IFCC RMPs 的正确实施情况和满足理想 APS(ALP、AST、LDH)或最佳 APS(ALT、CK、γGT)的可接受测量不确定度。还发现位于米兰和比得哥什的两个 Alinity 系统之间的所有酶测量均具有最佳的一致性。

结论 我们确认 Abbott Alinity c 分析系统上进行的 ALT、ALP、AST、CK、γGT 和 LDH 测量已正确标准化至 IFCC 参考测量系统,并且不同平台之间的系统一致性一致。

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