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儿童骨髓中末端脱氧核苷酸转移酶阳性淋巴前体细胞的四色流式细胞术研究:在早期B细胞发生过程中,CD79a表达先于CD19。

Four-color flow cytometric investigation of terminal deoxynucleotidyl transferase-positive lymphoid precursors in pediatric bone marrow: CD79a expression precedes CD19 in early B-cell ontogeny.

作者信息

Dworzak M N, Fritsch G, Fröschl G, Printz D, Gadner H

机构信息

Children's Cancer Research Institute, St Anna Kinderspital, Vienna, Austria.

出版信息

Blood. 1998 Nov 1;92(9):3203-9.

PMID:9787156
Abstract

Terminal deoxynucleotidyl transferase (TdT)-positive cells in human bone marrow (BM) are a phenotypically inhomogeneous population of precursor cells. In their majority, these TdT+ cells are unambiguously committed to the B lineage, as evidenced by CD19 expression. However, TdT+ precursors that lack CD19 also exist and these may encompass a differentiation potential for the B as well as for other lineages. Because recent data suggested that CD19 expression is not the earliest differentiation event in B-cell ontogeny, we sought to reevaluate TdT+ lymphoid precursors in pediatric BM to define the phenotypic denominator of B-lineage affiliation upstream of CD19. Using four-color flow cytometry, we focused on the assessment of the CD79a antigen, which is highly B-cell specific and which may also be expressed very early in B-cell ontogeny. We found that a majority of TdT+ cells coexpressed CD19 and CD79a in addition to CD10 and CD34, whereas, in all investigated samples, some TdT+ precursors lacked CD19 but expressed CD79a, which suggestively indicates also their B-lineage affiliation. In contrast to the CD19(+) precursors, which were usually CD10(hi) and CD79b+, these CD19(-)CD79a+ putative B-cell precursors preferentially expressed CD10 at low levels and were CD79b+ in only 41%. About 17% of these TdT+CD19(-)CD79a+ precursors also coexpressed CD33 and CD7, but not myeloperoxidase, CD14, or cytoplasmic CD3, which is discussed in the light of cellular activation rather than lineage promiscuity. Our data confirm that the earliest differentiation stages of B cells can be dissected upon expression of the lineage antigens CD79a and CD19 and imply that CD79a is earlier expressed than CD19. This raises the chance to follow the sequential events heralding B-cell commitment in the most immature precursors by correlating phenotypic and genetic differentiation markers.

摘要

人骨髓(BM)中末端脱氧核苷酸转移酶(TdT)阳性细胞是一群表型不均一的前体细胞。其中大多数TdT+细胞明确地定向于B淋巴细胞系,这可通过CD19表达得以证明。然而,缺乏CD19的TdT+前体细胞也存在,并且这些细胞可能具有向B淋巴细胞系以及其他细胞系分化的潜能。由于最近的数据表明CD19表达并非B细胞个体发生中最早的分化事件,我们试图重新评估儿科骨髓中的TdT+淋巴样前体细胞,以确定CD19上游B淋巴细胞系归属的表型标志。使用四色流式细胞术,我们重点评估了CD79a抗原,该抗原具有高度的B细胞特异性,并且也可能在B细胞个体发生的早期表达。我们发现,大多数TdT+细胞除了共表达CD10和CD34外,还共表达CD19和CD79a,而在所有研究样本中,一些TdT+前体细胞缺乏CD19但表达CD79a,这提示性地表明它们也属于B淋巴细胞系。与通常为CD10(高表达)和CD79b+的CD19(+)前体细胞不同,这些CD19(-)CD79a+假定的B细胞前体细胞优先低水平表达CD10,且仅41%为CD79b+。这些TdT+CD19(-)CD79a+前体细胞中约17%还共表达CD33和CD7,但不表达髓过氧化物酶、CD14或细胞质CD3,鉴于细胞活化而非谱系混杂对此进行了讨论。我们的数据证实,可根据谱系抗原CD79a和CD19的表达来剖析B细胞的最早分化阶段,并暗示CD79a比CD19更早表达。这增加了通过关联表型和基因分化标志物来追踪最不成熟前体细胞中预示B细胞定向的连续事件的机会。

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