Calibrating from Within: Multipoint Internal Calibration of a Quantitative Mass Spectrometric Assay of Serum Methotrexate

Author:

Hoffman Melissa A1,Schmeling Michael2,Dahlin Jayme L3,Bevins Nicholas J1,Cooper Donald P4,Jarolim Petr3,Fitzgerald Robert L1,Hoofnagle Andrew N2

Affiliation:

1. Department of Pathology, University of California San Diego School of Medicine, San Diego, CA

2. Department of Laboratory Medicine, University of Washington School of Medicine, Seattle, WA

3. Department of Pathology, Brigham and Women’s Hospital and Harvard Medical School, Boston, MA

4. Waters Corporation, Wilmslow, UK

Abstract

Abstract Background Clinical LC-MS/MS assays traditionally require that samples be run in batches with calibration curves in each batch. This approach is inefficient and presents a barrier to random access analysis. We developed an alternative approach called multipoint internal calibration (MPIC) that eliminated the need for batch-mode analysis. Methods The new approach used 4 variants of 13C-labeled methotrexate (0.026–10.3 µM) as an internal calibration curve within each sample. One site carried out a comprehensive validation, which included an evaluation of interferences and matrix effects, lower limit of quantification (LLOQ), and 20-day precision. Three sites evaluated assay precision and linearity. MPIC was also compared with traditional LC-MS/MS and an immunoassay. Results Recovery of spiked analyte was 93%–102%. The LLOQ was validated to be 0.017 µM. Total variability, determined in a 20-day experiment, was 11.5%CV. In a 5-day variability study performed at each site, total imprecision was 3.4 to 16.8%CV. Linearity was validated throughout the calibrator range (r2 > 0.995, slopes = 0.996–1.01). In comparing 40 samples run in each laboratory, the median interlaboratory imprecision was 6.55%CV. MPIC quantification was comparable to both traditional LC-MS/MS and immunoassay (r2 = 0.96–0.98, slopes = 1.04–1.06). Bland-Altman analysis of all comparisons showed biases rarely exceeding 20% when MTX concentrations were >0.4 µM. Conclusion The MPIC method for serum methotrexate quantification was validated in a multisite proof-of-concept study and represents a big step toward random-access LC-MS/MS analysis, which could change the paradigm of mass spectrometry in the clinical laboratory.

Funder

Waters Corp provided partial funding

Publisher

Oxford University Press (OUP)

Subject

Biochemistry (medical),Clinical Biochemistry

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