首页> 美国卫生研究院文献>Infection and Immunity >Human T helper cells specific for antigens of typhus group rickettsiae enhance natural killer cell activity in vitro.
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Human T helper cells specific for antigens of typhus group rickettsiae enhance natural killer cell activity in vitro.

机译:对斑疹伤寒立克次氏体抗原具有特异性的人T辅助细胞可增强体外的自然杀伤细胞活性。

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摘要

The peripheral blood mononuclear cells (PBMC) from 5 individuals immune to typhus group rickettsiae and from 13 nonimmune individuals were stimulated in vitro for 7 days with typhus group rickettsial antigen (TGRA). At the end of day 7, lysis of the natural killer (NK)-susceptible target K562 by these PBMC was determined. As controls, PBMC from both groups of donors were cultured in vitro for 7 days without antigen or were freshly isolated, and lysis of the K562 target was determined. There was no significant difference between the level of NK activity in freshly isolated PBMC from immune and nonimmune donors. PBMC from immune donors which were stimulated with antigen for 7 days exhibited significantly greater NK activity than did the control population, which was cultured for 7 days without antigen. PBMC from immune donors which were stimulated with TGRA demonstrated significantly higher NK activity than the same PBMC stimulated with antigen derived from an antigenically unrelated rickettsia, Coxiella burnetii. There was no significant difference, however, in the level of NK activity of nonimmune antigen-stimulated PBMC compared with that of the same PBMC population cultured without antigen. Most of the antigen-stimulated NK activity was mediated by Leu-11-positive cells as determined by electronic cell sorting. The ability of TGRA to sustain the NK activity of PBMC from immune donors was abolished when the T4/Leu-3-positive population of lymphocytes was eliminated by positive or negative selection prior to antigen stimulation. The ability of TGRA to sustain the NK activity of PBMC from immune donors was also significantly decreased in the presence of antibodies against human interleukin-2. The results suggest that the activity of human NK cells can be sustained in vitro by antigen-specific T helper cells and that the effect of the T helper cell is mediated, at least in part, by interleukin-2.
机译:用斑疹伤寒立克次体抗原(TGRA)体外刺激来自斑疹伤寒立克次氏体免疫的5个个体和13个非免疫个体的外周血单核细胞(PBMC)7天。在第7天结束时,确定了这些PBMC对天然杀伤(NK)敏感靶K562的裂解。作为对照,将来自两组供体的PBMC在无抗原的条件下体外培养7天或新鲜分离,并测定了K562靶的裂解。从免疫和非免疫供体新鲜分离的PBMC中,NK活性水平之间无显着差异。来自免疫供体的PBMC经抗原刺激7天后,其NK活性明显高于对照组,后者在无抗原的情况下培养7天。用TGRA刺激的免疫供体的PBMC表现出比用抗原无关的立克次氏体柯氏杆菌刺激的相同PBMC明显更高的NK活性。然而,与未抗原培养的相同PBMC群体相比,非免疫抗原刺激的PBMC的NK活性水平没有显着差异。如通过电子细胞分选所确定的,大多数抗原刺激的NK活性是由Leu-11-阳性细胞介导的。当在抗原刺激之前通过阳性或阴性选择消除了淋巴细胞的T4 / Leu-3阳性人群时,TGRA维持免疫供体的PBMC NK活性的能力就消失了。在存在针对人白介素2的抗体的情况下,TGRA维持免疫供体的PBMC NK NK活性的能力也显着降低。结果表明,人NK细胞的活性可以通过抗原特异性T辅助细胞在体外维持,并且T辅助细胞的作用至少部分是由白介素2介导的。

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