Clinical Significance of Serum Protein Electrophoresis in Rapid Progression of Multiple Myeloma: A Case Report.

IF 2.2 Q2 MEDICINE, GENERAL & INTERNAL

Clinics and Practice Pub Date : 2026-04-21 DOI:10.3390/clinpract16040081

Silvia Iannelli, Melania Scarcella, Antonella Cusano, Federica Feleppa, Ylenia Pancione, Luigi Michele Pavone, Pasquale Cocchiaro

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Abstract

Background/Objectives: Serum protein electrophoresis (SPE) is a widely used laboratory test for the detection and monitoring of monoclonal gammopathies, including multiple myeloma (MM). Although SPE is usually recommended in the presence of specific clinical or laboratory abnormalities, monoclonal gammopathies may occasionally develop rapidly and without typical symptoms. This case report aims to emphasize the diagnostic value of SPE in identifying an unexpected and fast-evolving monoclonal gammopathy. Methods: We report the clinical and laboratory eight-month follow-up of a 58-year-old male who initially underwent SPE for unrelated clinical conditions. Serial SPE analyses were performed using capillary zone electrophoresis. When abnormalities emerged, immunotyping and serum free light chain (FLC) assays were conducted. The diagnostic workup was completed with bone marrow aspiration, flow cytometry, and imaging studies according to current international diagnostic criteria. Results: The initial SPE (November 2023) showed a normal protein profile. After eight months, follow-up SPE revealed a prominent monoclonal spike in the gamma region (2.9 g/dL), associated with increased total serum proteins (91 g/L; range 64-82 g/L), elevated IgA levels (20.0 g/L; range 0.4-3.5 g/L), and a markedly abnormal κ/λ FLC ratio (54.00; range 0.31-1.56). Bone marrow analysis demonstrated >18% plasma cell infiltration, confirming the diagnosis of IgA-κ MM. The patient underwent standard therapy followed by autologous stem cell transplantation, achieving disease remission. Conclusions: This case highlights that clinically relevant monoclonal gammopathies may arise rapidly in the absence of classical diagnostic features. Routine SPE represents a cost-effective and accessible screening tool that can identify subtle protein abnormalities, prompting the timely use of more specific and invasive diagnostic procedures for aggressive plasma cell disorders.

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血清蛋白电泳在多发性骨髓瘤快速进展中的临床意义1例报告。

背景/目的：血清蛋白电泳（SPE）是一种广泛用于检测和监测单克隆伽玛病的实验室检测方法，包括多发性骨髓瘤（MM）。尽管SPE通常在存在特定临床或实验室异常时推荐使用，但单克隆伽玛病偶尔也会迅速发展且无典型症状。本病例报告旨在强调SPE在识别意外和快速发展的单克隆伽玛病方面的诊断价值。方法：我们报告了一名58岁男性的临床和实验室8个月的随访，他最初因不相关的临床疾病接受了SPE。采用毛细管区带电泳进行固相萃取分析。当出现异常时，进行免疫分型和血清游离轻链（FLC）测定。根据目前的国际诊断标准，通过骨髓穿刺、流式细胞术和影像学检查完成诊断工作。结果：最初的SPE（2023年11月）显示正常的蛋白质谱。8个月后，随访的SPE显示γ区有明显的单克隆峰（2.9 g/dL），与血清总蛋白升高（91 g/L，范围64-82 g/L）、IgA水平升高（20.0 g/L，范围0.4-3.5 g/L）和κ/λ FLC比值明显异常（54.00，范围0.31-1.56）相关。骨髓分析显示>18%浆细胞浸润，证实IgA-κ MM的诊断。患者接受标准治疗后进行自体干细胞移植，病情缓解。结论：该病例强调在缺乏经典诊断特征的情况下，临床相关的单克隆伽玛病可能会迅速出现。常规SPE是一种具有成本效益和可获得的筛查工具，可以识别细微的蛋白质异常，促进对侵袭性浆细胞疾病及时使用更具体和侵入性的诊断程序。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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