AI Article Synopsis

  • New immunoglobulin free light chain (FLC) assays, including FreeLite and Sebia, can be used interchangeably for diagnosing multiple myeloma and assessing risk in patients with MGUS, despite differing methodologies.
  • A study of 923 MGUS patients showed that both assays had comparable effectiveness in predicting progression to plasma cell dyscrasias (PCD) over a median follow-up of 38 years.
  • The Sebia assay offered improved risk stratification with a lower clinical decision point for patients with low FLC ratios, demonstrating the potential for its application alongside traditional models.

Article Abstract

Background: New immunoglobulin free light chain (FLC) assays are available. Despite analytical differences, it seems possible to use free light chain ratios (FLCr) generated by different assays and apply similar cut-points for the diagnosis of multiple myeloma. It is still unknown if we can use different assays for risk stratification of patients with monoclonal gammopathy of undetermined significance (MGUS).

Methods: Patients diagnosed with MGUS (N = 923) had FLC tested using a nephelometric FreeLite (Binding Site) assay on BNII instruments (Siemens) and a Sebia FLC assay (Sebia) on a DS2 ELISA analyzer (Dynex). Patients were followed up for progression to any plasma cell dyscrasia (PCD) for several decades. The Mayo MGUS risk stratification model for progression was assessed with both assays (M-spike >1.5 g/dL; non-IgG isotype and abnormal FLCr), using package insert reference intervals (RI) and a new metric called principal component 2 (PC2).

Results: There were 94 events of progression to PCD in the cohort during a median of 38 years of follow-up. Freelite and Sebia FLC showed similar hazard ratios in the risk models for elevated FLCr. An alternative clinical decision point lower than the package insert RI was evaluated for the Sebia assay, which improved risk stratification for patients with a low FLCr. The PC2 metric showed similar performance to the FLCr in models, without superior benefit.

Conclusions: The Sebia ELISA-based FLC assay can be employed in an MGUS risk stratification model with similar performance to the original 2005 risk stratification model using the FreeLite assay.

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Source
http://dx.doi.org/10.1093/clinchem/hvae124DOI Listing

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