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利用成年骨髓基质对14.5天龄小鼠胎肝中自然杀伤细胞发育阶段的特征分析。

Characterization of the stage in natural killer cell development in 14.5-day mouse fetal liver using adult bone marrow stroma.

作者信息

Lu J, Patrene K D, Appasamy P M, Herberman R B, Boggs S S

机构信息

Department of Radiation Oncology, University of Pittsburgh School of Medicine, and University of Pittsburgh Cancer Institute, PA, USA.

出版信息

Exp Hematol. 1999 Jun;27(6):1046-56. doi: 10.1016/s0301-472x(99)00042-9.

Abstract

Nonstimulated fetal liver (FL) from 14.5-day gestation mice had no natural killer (NK) cell activity and <3% expressed NK1.1. Even after short-term (3-4 day) culture of FL with the late-acting cytokines, interleukin (IL)-15 or IL-2, little or no NK activity was detected. However, longer-term (13 day) culture with IL-2 plus stroma derived from bone marrow (BM) of adult mice, resulted in extensive proliferation and differentiation to mature NK cells. Cell numbers began to increase after 4 days, and by day 13, they had increased 40-fold and 69% of the cells were NK1.1+ with high NK activity and 5%-10% were NK1.1- B220+. With stroma, but no IL-2, equivalent proliferation occurred, but differentiated cells were predominantly NK1.1- B220+, not NK cells. Culture for 13 days without stroma, but with either IL-2, IL-15, FLTK3-ligand (L) or stroma-conditioned medium, resulted in less than fivefold expansion, and minimal NK activity. Culture with combinations of FLTK3-L or ckit-L plus IL-15 or IL-2 increased both cell number and NK activity, but the increase in cell number was less than that seen with stroma plus IL-2. By limiting dilution assay on stroma plus IL-2, the precursor frequency was 1/(2660+/-292) whole FL cells and the absolute number, but not the frequency, increased during culture on stroma without IL-2. The NK cell progenitors were found in sorted NK1.1- and Sca-1+ c-kit+ lineage- subpopulations at a frequency of 1/(156+/-52.5). Together, these data suggest that the NK lineage cells in FL are primarily in early stages of development. They are highly proliferative, respond to early acting cytokines and express stem cell markers.

摘要

来自妊娠14.5天小鼠的未刺激胎儿肝脏(FL)没有自然杀伤(NK)细胞活性,且表达NK1.1的细胞少于3%。即使将FL与晚期作用细胞因子白细胞介素(IL)-15或IL-2进行短期(3 - 4天)培养,也检测到很少或没有NK活性。然而,用IL-2加上成年小鼠骨髓(BM)来源的基质进行长期(13天)培养,会导致大量增殖并分化为成熟NK细胞。细胞数量在4天后开始增加,到第13天,增加了40倍,69%的细胞为NK1.1 +且具有高NK活性,5% - 10%为NK1.1 - B220 +。有基质但无IL-2时,发生了同等程度的增殖,但分化细胞主要是NK1.1 - B220 +,而非NK细胞。在无基质但有IL-2、IL-15、FLTK3配体(L)或基质条件培养基的情况下培养13天,导致细胞扩增不到五倍,且NK活性极低。用FLTK3 - L或ckit - L与IL-15或IL-2组合培养可增加细胞数量和NK活性,但细胞数量的增加少于基质加IL-2的情况。通过对基质加IL-2进行有限稀释分析,前体频率为1/(2660±292)个全FL细胞,在无IL-2的基质上培养期间,绝对细胞数增加,但频率未增加。在分选的NK1.1 -和Sca - 1 + c - kit +谱系 -亚群中发现NK细胞祖细胞,频率为1/(156±52.5)。总之,这些数据表明FL中的NK谱系细胞主要处于发育早期阶段。它们具有高度增殖性,对早期作用细胞因子有反应,并表达干细胞标志物。

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