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鉴定出一种新型人类脐带血CD34-CD133-CD7-CD45+谱系阴性细胞亚群,该亚群在体外暴露于白细胞介素-15后能够分化为淋巴细胞/NK细胞。

Identification of a novel subpopulation of human cord blood CD34-CD133-CD7-CD45+lineage- cells capable of lymphoid/NK cell differentiation after in vitro exposure to IL-15.

作者信息

Rutella Sergio, Bonanno Giuseppina, Marone Maria, De Ritis Daniela, Mariotti Andrea, Voso Maria Teresa, Scambia Giovanni, Mancuso Salvatore, Leone Giuseppe, Pierelli Luca

机构信息

Department of Hematology, Laboratory of Immunology, Catholic University Medical School, Rome, Italy.

出版信息

J Immunol. 2003 Sep 15;171(6):2977-88. doi: 10.4049/jimmunol.171.6.2977.

Abstract

The hemopoietic stem cell (HSC) compartment encompasses cell subsets with heterogeneous proliferative and developmental potential. Numerous CD34(-) cell subsets that might reside at an earlier stage of differentiation than CD34(+) HSCs have been described and characterized within human umbilical cord blood (UCB). We identified a novel subpopulation of CD34(-)CD133(-)CD7(-)CD45(dim)lineage (lin)(-) HSCs contained within human UCB that were endowed with low but measurable extended long-term culture-initiating cell activity. Exposure of CD34(-)CD133(-)CD7(-)CD45(dim)lin(-) HSCs to stem cell factor preserved cell viability and was associated with the following: 1) concordant expression of the stem cell-associated Ags CD34 and CD133, 2) generation of CFU-granulocyte-macrophage, burst-forming unit erythroid, and megakaryocytic aggregates, 3) significant extended long-term culture-initiating cell activity, and 4) up-regulation of mRNA signals for myeloperoxidase. At variance with CD34(+)lin(-) cells, CD34(-)CD133(-)CD7(-)CD45(dim)lin(-) HSCs maintained with IL-15, but not with IL-2 or IL-7, proliferated vigorously and differentiated into a homogeneous population of CD7(+)CD45(bright)CD25(+)CD44(+) lymphoid progenitors with high expression of the T cell-associated transcription factor GATA-3. Although they harbored nonclonally rearranged TCRgamma genes, IL-15-primed CD34(-)CD133(-)CD7(-)CD45(dim)lin(-) HSCs failed to achieve full maturation, as manifested in their CD3(-)TCRalphabeta(-)gammadelta(-) phenotype. Conversely, culture on stromal cells supplemented with IL-15 was associated with the acquisition of phenotypic and functional features of NK cells. Collectively, CD34(-)CD133(-)CD7(-)CD45(dim)lin(-) HSCs from human UCB displayed an exquisite sensitivity to IL-15 and differentiated into lymphoid/NK cells. Whether the transplantation of CD34(-)lin(-) HSCs possessing T/NK cell differentiation potential may impact on immunological reconstitution and control of minimal residual disease after HSC transplantation for autoimmune or malignant diseases remains to be determined.

摘要

造血干细胞(HSC)区室包含具有异质性增殖和发育潜能的细胞亚群。在人脐带血(UCB)中已描述并鉴定了许多可能比CD34(+)造血干细胞处于更早分化阶段的CD34(-)细胞亚群。我们在人UCB中鉴定出一种新的CD34(-)CD133(-)CD7(-)CD45(dim)谱系(lin)(-)造血干细胞亚群,其具有低但可测量的长期培养起始细胞活性。将CD34(-)CD133(-)CD7(-)CD45(dim)lin(-)造血干细胞暴露于干细胞因子可维持细胞活力,并与以下情况相关:1)干细胞相关抗原CD34和CD133的协同表达;2)产生集落形成单位-粒细胞-巨噬细胞、爆式红系集落形成单位和巨核细胞集落;3)显著延长的长期培养起始细胞活性;4)髓过氧化物酶mRNA信号的上调。与CD34(+)lin(-)细胞不同,用IL-15而非IL-2或IL-7培养的CD34(-)CD133(-)CD7(-)CD45(dim)lin(-)造血干细胞能旺盛增殖,并分化为均一的高表达T细胞相关转录因子GATA-3的CD7(+)CD45(bright)CD25(+)CD44(+)淋巴祖细胞群。尽管它们含有非克隆重排的TCRγ基因,但IL-15预处理的CD34(-)CD133(-)CD7(-)CD45(dim)lin(-)造血干细胞未能完全成熟,这表现为它们的CD3(-)TCRαβ(-)γδ(-)表型。相反,在补充有IL-15的基质细胞上培养与获得NK细胞的表型和功能特征相关。总体而言,人UCB中的CD34(-)CD133(-)CD7(-)CD45(dim)lin(-)造血干细胞对IL-15表现出极高的敏感性,并分化为淋巴样/NK细胞。具有T/NK细胞分化潜能的CD34(-)lin(-)造血干细胞移植是否会影响自身免疫性疾病或恶性疾病造血干细胞移植后的免疫重建和微小残留病的控制仍有待确定。

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