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人外周血树突状细胞亚群。前体和成熟抗原呈递细胞的分离与鉴定。

Human peripheral blood dendritic cell subsets. Isolation and characterization of precursor and mature antigen-presenting cells.

作者信息

Thomas R, Lipsky P E

机构信息

Harold C. Simmons Arthritis Research Center, University of Texas Southwestern Medical School, Dallas 75235.

出版信息

J Immunol. 1994 Nov 1;153(9):4016-28.

PMID:7523513
Abstract

Dendritic cells (DC) are the major APC capable of stimulating resting T cells in human peripheral blood (PB). Recent evidence suggested that various subsets of DC and monocytes might circulate in human PB, but their exact phenotype and function had not been delineated. We have previously characterized a population of human PB DC precursors that express the myeloid marker CD33, but not the monocyte marker CD14. To identify and characterize further functional myeloid APC subsets, triple color FACS analysis and sorting was used. A CD33dimCD14dimCD16+ monocyte subset, with similar APC function but less efficient accessory function than CD14bright monocytes, was isolated. In addition to the CD33+CD14dimCD16- DC precursors, a smaller population (0.1 to 0.2% of PBMC) of CD33brightCD14dimCD16- cells with potent APC function was identified. This DC population expressed greater amounts of MHC class II, adhesion, and accessory molecules, and demonstrated a greater costimulatory capacity when freshly isolated than CD33dimCD14dim DC precursors, and therefore had the characteristics of mature, possibly tissue-derived DC. When freshly isolated, however, these DC did not express B7, and up-regulation of accessory function occurred after in vitro differentiation. These data demonstrate multiple circulating myeloid accessory and APC subsets in human PB. Phenotypic and functional differences suggest that they are at different stages of differentiation, and have specialized roles in Ag presentation in vivo. Furthermore, full functional DC differentiation, associated with B7 expression and the capacity to activate T cells maximally, is likely to occur only in specific physiologic circumstances.

摘要

树突状细胞(DC)是能够刺激人外周血(PB)中静止T细胞的主要抗原呈递细胞(APC)。最近的证据表明,DC和单核细胞的各种亚群可能在人PB中循环,但它们的确切表型和功能尚未明确。我们之前已对一群表达髓系标志物CD33但不表达单核细胞标志物CD14的人PB DC前体进行了特征描述。为了进一步鉴定和表征功能性髓系APC亚群,我们采用了三色荧光激活细胞分选术(FACS)分析和分选。分离出了一个CD33dimCD14dimCD16+单核细胞亚群,其APC功能与CD14bright单核细胞相似,但辅助功能较弱。除了CD33+CD14dimCD16- DC前体,还鉴定出了一小群(占外周血单个核细胞的0.1%至0.2%)具有强大APC功能的CD33brightCD14dimCD16-细胞。与CD33dimCD14dim DC前体相比,这群DC表达了更多的MHC II类分子、黏附分子和辅助分子,并且在刚分离时表现出更强的共刺激能力,因此具有成熟的、可能来源于组织的DC的特征。然而,刚分离时,这些DC不表达B7,其辅助功能在体外分化后上调。这些数据证明了人PB中存在多种循环的髓系辅助细胞和APC亚群。表型和功能上的差异表明它们处于不同的分化阶段,并且在体内抗原呈递中具有特定作用。此外,与B7表达以及最大程度激活T细胞的能力相关的完全功能性DC分化可能仅在特定的生理情况下发生。

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