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人类骨髓正常造血的免疫表型分化模式:年龄相关变化和疾病诱导转变的参考模式

Immunophenotypic differentiation patterns of normal hematopoiesis in human bone marrow: reference patterns for age-related changes and disease-induced shifts.

作者信息

van Lochem E G, van der Velden V H J, Wind H K, te Marvelde J G, Westerdaal N A C, van Dongen J J M

机构信息

Department of Immunology, Erasmus MC, University Medical Center Rotterdam, Rotterdam, The Netherlands.

出版信息

Cytometry B Clin Cytom. 2004 Jul;60(1):1-13. doi: 10.1002/cyto.b.20008.

Abstract

BACKGROUND

The abundance of monoclonal antibodies (mAb) and the routine use of quadruple stainings in flow cytometry allow stepwise analysis of bone marrow (BM) samples that are suspected for abnormal hematopoiesis. A screening phase that precedes lineage-specific classification phases should be sufficient to assess whether the BM has a normal or abnormal composition, as well as to identify the abnormal differentiation lineage.

METHODS

For a quick and easy flow cytometric screening of BM samples, we selected six quadruple immunostainings that cover multiple differentiation stages of the B-cell, monocytic, granulocytic, and erythroid lineages: TdT/CD20/CD19/CD10 and CD45/CD34/CD19/CD22 for B cells, CD34/CD117/CD45/CD13.33 for precursor granulocytic and precursor monocytic cells (myelo/monoblasts), CD14/CD33/CD45/CD34 for monocytic cells, CD16/CD13/CD45/CD11b for granulocytic cells, and CD71/CD235a/CD45/CD117 for erythroid cells.

RESULTS

The six quadruple immunostainings reveal specific staining patterns in normal BM, which allow the recognition of various subpopulations of the respective lineages. These staining patterns can be used as a frame of reference for recognition of normal and abnormal BM development. Examples of normal (age-related) variations in these otherwise stable staining patterns are presented together with several abnormal differentiation patterns.

CONCLUSIONS

Although alternative immunostainings can be used (e.g., including NK- and T-cell markers), we feel that the selected six stainings represent a comprehensive and easy screening phase for quick identification of shifts in the composition of the studied differentiation lineages, reflecting age-related changes or disease-induced BM abnormalities.

摘要

背景

单克隆抗体(mAb)种类丰富,且流式细胞术中四重染色的常规应用使得对怀疑存在异常造血的骨髓(BM)样本进行逐步分析成为可能。在特定谱系分类阶段之前的筛查阶段应足以评估骨髓组成是否正常或异常,并识别异常分化谱系。

方法

为了对骨髓样本进行快速简便的流式细胞术筛查,我们选择了六种四重免疫染色,它们覆盖了B细胞、单核细胞、粒细胞和红系谱系的多个分化阶段:用于B细胞的TdT/CD20/CD19/CD10和CD45/CD34/CD19/CD22,用于前体粒细胞和前体单核细胞(髓母细胞/单核母细胞)的CD34/CD117/CD45/CD13.33,用于单核细胞的CD14/CD33/CD45/CD34,用于粒细胞的CD16/CD13/CD45/CD11b,以及用于红系细胞的CD71/CD235a/CD45/CD117。

结果

这六种四重免疫染色揭示了正常骨髓中的特定染色模式,从而能够识别各个谱系的不同亚群。这些染色模式可作为识别正常和异常骨髓发育的参考框架。本文展示了这些原本稳定的染色模式中正常(与年龄相关)变化的实例以及几种异常分化模式。

结论

尽管可以使用其他免疫染色(例如,包括NK和T细胞标志物),但我们认为所选的六种染色代表了一个全面且简便的筛查阶段,可快速识别所研究分化谱系组成的变化,反映与年龄相关的变化或疾病引起的骨髓异常。

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