Evaluation of routine laboratory parameters as clinical indicators of disease severity in multiple myeloma
Batuhan Subasi1, Nahide Ekici Gunay1, Derya Kocer1, Esra Yildizhan21Department of Medical Biochemistry, Kayseri City Training and Research Hospital, Kayseri, Türkiye2Department of Medical Hematology, Kayseri City Training and Research Hospital, Kayseri, Türkiye
INTRODUCTION: Multiple myeloma (MM) is characterized by clonal plasma cell proliferation and significant systemic im-pacts. This study aimed to evaluate the relationship between routine hemogram and biochemical parameters and disease severity markers (M-protein and β-2 microglobulin [β-2M]) to identify accessible clinical indicators of tumor load at the time of diagnosis.
METHODS: In this retrospective cross-sectional study, newly diagnosed, treatment-naive MM patients and healthy con-trols were analyzed. Statistical significance was set at a threshold (p<0.00125) using Bonferroni correction to prevent Type I errors. Multivariable logistic regression was performed to identify independent predictors of high M-protein load (≥3g/dL), and ROC analysis was used to determine the diagnostic performance of significant parameters.
RESULTS: MM patients exhibited significantly lower WBC, RBC, HCT, and PLT counts, and higher BUN and CRP levels compared to controls (p<0.001). β-2M showed significant correlations with several routine parameters; however, partial correlation and multivariable regression revealed that these associations were entirely dependent on renal function. Conversely, multivariable logistic regression identified RBC count (OR=0.383, p=0.026), eGFR, and age as significant in-dependent predictors of high M-protein load. Notably, each 1×10⁶/μL decline in RBC count was associated with a 161% increase in the risk of high disease severity. ROC analysis established an optimal RBC cut-off value of 3.73×10⁶/μL (AUC: 0.695, sensitivity: 64.1%, specificity: 69.6%) for predicting high tumor load.
DISCUSSION AND CONCLUSION: Routine laboratory data, particularly RBC count, serve as powerful indicators of MM severity at the time of initial diagnosis. Unlike β-2M, which is heavily influenced by renal status, RBC count is an independent predictor of monoclonal protein load. A baseline RBC level below 3.73×10⁶/μL should alert clinicians to a potentially high tumor load, facilitating rapid triage and treatment prioritization.
Keywords: Beta 2-microglobulin, complete blood count, C-reactive protein, multiple myeloma, paraproteins
Manuscript Language: English