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常规实验室是否应停止进行血清蛋白电泳筛查,转而采用免疫固定电泳筛查?没有快速解决办法:反对意见。

Should routine laboratories stop doing screening serum protein electrophoresis and replace it with screening immune-fixation electrophoresis? No quick fixes: Counterpoint.

出版信息

Clin Chem Lab Med. 2016 Jun 1;54(6):967-71. doi: 10.1515/cclm-2015-0806.

Abstract

Monoclonal gammopathies are characterised by the production of a monoclonal immunoglobulin or free light chains by an abnormal plasma cell or B-cell clone and may indicate malignancy or a precursor (MGUS). There is currently no consensus on the initial test or combination of tests to be performed in suspected monoclonal gammopathies but serum protein electrophoresis and urine protein electrophoresis are commonly requested as initial investigations. If abnormal, immunofixation electrophoresis is then performed to confirm the presence of paraprotein and to determine its heavy and light chain type. Recently, some groups have developed simplified "screening" IFE methods for use in parallel to SPEP for the detection monoclonal gammopathies. We argue here that screening IFE may be of benefit in clinical laboratories using SPEP with poor resolution in the β-region, assisting in the detection of mainly IgA paraprotein, but may be of less benefit in laboratories utilising higher resolution gels. Further it may increase the detection of trace bands of questionable clinical significance, representing transient phenomena in infectious and auto-immune conditions or very low risk MGUS. The increased detection of these bands using screening IFE would require further patient follow up, possibly causing unnecessary patient anxiety and additional follow up healthcare costs.

摘要

单克隆丙种球蛋白病的特征是由异常浆细胞或 B 细胞克隆产生单克隆免疫球蛋白或游离轻链,可能提示恶性肿瘤或前体(MGUS)。目前对于疑似单克隆丙种球蛋白病应进行的初始检查或联合检查尚无共识,但血清蛋白电泳和尿蛋白电泳通常作为初始检查要求。如果异常,则进行免疫固定电泳以确认存在副蛋白,并确定其重链和轻链类型。最近,一些小组已经开发了简化的“筛查”IFE 方法,与 SPEP 平行使用,用于检测单克隆丙种球蛋白病。我们认为,在使用 SPEP 时分辨率较差的临床实验室中,筛查 IFE 可能有益,有助于检测主要的 IgA 副蛋白,但在使用分辨率更高的凝胶的实验室中可能益处较小。此外,它可能会增加对有疑问的临床意义的痕量带的检测,这些痕量带代表感染和自身免疫性疾病中的瞬时现象或风险极低的 MGUS。使用筛查 IFE 检测到这些带可能需要进一步的患者随访,可能导致不必要的患者焦虑和额外的后续医疗保健费用。

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