| Literature DB >> 28573706 |
Jennifer L J Heaney1, John P Campbell1, Anne E Griffin1, Jane Birtwistle1, Meena Shemar2, J Anthony Child3, Walter M Gregory3, David A Cairns3, Gareth Morgan4, Graham Jackson5, Mark T Drayson1.
Abstract
This study aims to guide the integration of serum free light chain (sFLC) tests into clinical practice, including a new rapid test (Seralite® ). Blood and urine analysis from 5573 newly diagnosed myeloma patients identified 576 light chain only (LCO) and 60 non-secretory (NS) cases. Serum was tested by Freelite® and Seralite® at diagnosis, maximum response and relapse. 20% of LCO patients had urine FLC levels below that recommended for measuring response but >97% of these had adequate sFLC levels (oligosecretory). The recommended Freelite® sFLC ≥100 mg/l for measuring response was confirmed and the equivalent Seralite® FLC difference (dFLC) >20 mg/l identified. By both methods, ≥38% of NS patients had measurable disease (oligosecretory). Higher sFLC levels were observed on Freelite® at all time points. However, good clinical concordance was observed at diagnosis and in response to therapy. Achieving at least a very good partial response according to either sFLC method was associated with better patient survival. Relapse was identified using a Freelite® sFLC increase >200 mg/l and found 100% concordance with a corresponding Seralite® dFLC increase >30 mg/l. Both Freelite® and Seralite® sensitively diagnose and monitor LCO/oligosecretory myeloma. Rapid testing by Seralite® could fast-track FLC screening and monitoring. Response by sFLC assessment was prognostic for survival and demonstrates the clinical value of routine sFLC testing.Entities:
Keywords: free light chains; multiple myeloma; non-secretory; quantitation; serum; survival
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Year: 2017 PMID: 28573706 DOI: 10.1111/bjh.14753
Source DB: PubMed Journal: Br J Haematol ISSN: 0007-1048 Impact factor: 6.998