An international multi-center serum protein electrophoresis accuracy and M-protein isotyping study. Part II: limit of detection and follow-up of patients with small M-proteins-Reference-Cited by-同舟云学术

An international multi-center serum protein electrophoresis accuracy and M-protein isotyping study. Part II: limit of detection and follow-up of patients with small M-proteins

Published:2020-01-15 Issue:4 Volume:58 Page:547-559
ISSN:1437-4331
Container-title:Clinical Chemistry and Laboratory Medicine (CCLM)
language:en
Short-container-title:

Author:

Jacobs Joannes F.M.¹,Turner Katherine A.²,Graziani Maria Stella³,Frinack Jody L.²,Ettore Michael W.²,Tate Jillian R.⁴,Booth Ronald A.⁵,McCudden Christopher R.⁵,Keren David F.⁶,Delgado Julio C.⁷,Zemtsovskaja Galina⁸,Fullinfaw Robert O.⁹,Caldini Anna¹⁰,de Malmanche Theo¹¹,Katakouzinos Katina¹²,Burke Matthew⁴,Palladini Giovanni¹³,Altinier Sara¹⁴,Zaninotto Martina¹⁴,Righetti Gabriella¹⁵,Melki Marie Therese¹⁶,Bell Stephen¹⁷,Willrich Maria Alice Vieira¹⁸

Affiliation:

1. Laboratory Medical Immunology, Department of Laboratory Medicine , Radboud University Medical Center , Geert Grooteplein 10 , 6525 GA Nijmegen , The Netherlands

2. Department of Laboratory Medicine and Pathology , Mayo Clinic , Rochester , MN , USA

3. Section of Clinical Biochemistry , University of Verona , Verona , Italy

4. Department of Chemical Pathology , Pathology Queensland, Royal Brisbane and Women’s Hospital , Brisbane , QLD , Australia

5. Department of Pathology and Laboratory Medicine , The Ottawa Hospital , Ottawa , ON , Canada

6. Department of Pathology , The University of Michigan , Ann Arbor , MI , USA

7. ARUP Laboratories, Department of Pathology , University of Utah School of Medicine , Salt Lake City , UT , USA

8. Clinical Chemistry Laboratory , North Estonia Medical Centre , Tallinn , Estonia

9. Department of Chemical Pathology , The Royal Melbourne Hospital , Melbourne, Victoria , Australia

10. General Laboratory , Careggi University Hospital , Florence , Italy

11. NSW Health Pathology, Immunology Department , John Hunter Hospital , New Lambton Heights NSW , Australia

12. Immunopathology Department , Royal Prince Alfred Hospital , Camperdown , NSW , Australia

13. Amyloidosis Research and Treatment Center, Foundation IRCCS Policlinico San Matteo, and Department of Molecular Medicine, University of Pavia , Pavia , Italy

14. Laboratory Medicine of the University Hospital of Padova , Padova , Italy

15. Clinical Chemistry Laboratory , University of Verona , Verona , Italy

16. Sebia Inc. , Lisses , France

17. Helena Biosciences Europe , Sunderland , UK

18. Division of Clinical Biochemistry and Immunology, Department of Laboratory Medicine and Pathology , Mayo Clinic , 200 First Street SW , Rochester, MN 55905 , USA

Abstract

Abstract Background Electrophoretic methods to detect, characterize and quantify M-proteins play an important role in the management of patients with monoclonal gammopathies (MGs). Significant uncertainty in the quantification and limit of detection (LOD) is documented when M-proteins are <10 g/L. Using spiked sera, we aimed to assess the variability in intact M-protein quantification and LOD across 16 laboratories. Methods Sera with normal, hypo- or hyper-gammaglobulinemia were spiked with daratumumab or elotuzumab, with concentrations from 0.125 to 10 g/L (n = 62) along with a beta-migrating sample (n = 9). Laboratories blindly analyzed samples according to their serum protein electrophoresis (SPEP)/isotyping standard operating procedures. LOD and intra-laboratory percent coefficient of variation (%CV) were calculated and further specified with regard to the method (gel/capillary electrophoresis [CZE]), gating strategy (perpendicular drop [PD]/tangent skimming [TS]), isotyping (immunofixation/immunosubtraction [ISUB]) and manufacturer (Helena/Sebia). Results All M-proteins ≥1 g/L were detected by SPEP. With isotyping the LOD was moderately more sensitive than with SPEP. The intensity of polyclonal background had the biggest negative impact on LOD. Independent of the method used, the intra-laboratory imprecision of M-protein quantification was small (mean CV = 5.0%). Low M-protein concentration and high polyclonal background had the strongest negative impact on intra-laboratory precision. All laboratories were able to follow trend of M-protein concentrations down to 1 g/L. Conclusions In this study, we describe a large variation in the reported LOD for both SPEP and isotyping; overall LOD is most affected by the polyclonal immunoglobulin background. Satisfactory intra-laboratory precision was demonstrated. This indicates that the quantification of small M-proteins to monitor patients over time is appropriate, when subsequent testing is performed within the same laboratory.

Publisher

Walter de Gruyter GmbH

Subject

Biochemistry (medical),Clinical Biochemistry,General Medicine

Link

https://www.degruyter.com/document/doi/10.1515/cclm-2019-1105/pdf

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