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首页> 外文期刊>American journal of clinical pathology. >Utility of nine-color, 11-Parameter flow cytometry for detection of plasma cell neoplasms: A comparison with bone marrow morphologic findings and concurrent M-protein studies in serum and urine
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Utility of nine-color, 11-Parameter flow cytometry for detection of plasma cell neoplasms: A comparison with bone marrow morphologic findings and concurrent M-protein studies in serum and urine

机译:九色,十一参数流式细胞仪用于浆细胞肿瘤的检测:与骨髓形态学发现和血清和尿液中同时进行的M蛋白研究的比较

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摘要

Objectives: Multiparameter flow cytometry (MFC) is a widely available laboratory platform for the evaluation of plasma cell (PC) neoplasms. We assess the performance of a nine-color MFC assay that uses stain-lyse-fix processing of bone marrow aspirates, minimal wash steps, and high acquisition rates with analysis of up to 1.8 × 106cells.Methods: MFC results were compared with microscopic examinations, immunohistochemical studies, and serum/urine M-protein measurements from patients with documented or suspected PC neoplasms.Results: Sensitivity exceeded that of microscopic examinations, with or without immunohistochemistry. In patients with PC myeloma, clonal PC detection by MFC fell in concert with M-protein levels. However, in a subset of patients, MFC detected clonal PCs after serum/urine studies turned negative.Conclusions: The nine-color analytic cocktail eliminates duplication of PC gating reagents required for evaluation of the same epitopes using a five- or six-color approach. Fewer analytic cocktails result in lower instrument acquisition times per case, a significant factor for the large data sets required for optimal residual disease assessment. Finally, concurrent analysis of nine epitopes and two light scatter parameters aids detection of residual disease, particularly when it is mixed with polyclonal PCs.
机译:目的:多参数流式细胞术(MFC)是广泛用于评估浆细胞(PC)肿瘤的实验室平台。我们评估了一种九色MFC分析的性能,该分析使用了骨髓抽吸物的染色-裂解固定处理,最少的洗涤步骤和高达1.8×106个细胞的分析的高采集率。方法:将MFC结果与显微镜检查进行比较,有组织的或疑似PC肿瘤患者的免疫组化研究,血清/尿M蛋白测量。结果:无论是否进行免疫组化,敏感性均超过镜检。在PC骨髓瘤患者中,MFC进行的克隆PC检测与M蛋白水平一致。然而,在部分患者中,MFC在血清/尿液研究转为阴性后检测到了克隆PC。结论:九色分析混合物消除了使用五色或六色方法评估相同表位所需的PC门控试剂的重复。 。较少的分析混合物可使每个案例的仪器获取时间缩短,这对于进行最佳残留疾病评估所需的大量数据集是一个重要因素。最后,同时分析9个表位和2个光散射参数有助于检测残留疾病,尤其是与多克隆PC混合使用时。

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