von der Weid T, Beebe A M, Roopenian D C, Coffman R L
Department of Immunology, DNAX Research Institute of Molecular and Cellular Biology, Palo Alto, CA 94304, USA.
J Immunol. 1996 Nov 15;157(10):4421-7.
Splenic CD4+NK1.1+ T cells have been shown to secrete large and transient amounts of IL-4 mRNA 90 min after i.v. injection of anti-CD3 Ab, suggesting that this novel subset of T cells may induce Th2 responses in the spleen by quickly providing IL-4 at the onset of an immune response. beta2-microglobulin-deficient (beta2m(o/o)) mice have been shown to contain strongly reduced numbers of NK1.1+ T cells and to be severely impaired in their capacity for rapid induction of IL-4 mRNA in response to anti-CD3, demonstrating that these cells are MHC class I dependent. To address the role of CD4+NK1.1+ T cells in the induction of Th2 responses against Leishmania major, we have dissected the onset and the outcome of the immune response elicited against the parasite in BALB/c-beta2m(o/o) mice and in anti-NK1.1-treated congenic BALB/c mice expressing the NK1.1 marker (BALB/c-NK1.1+). Both BALB/c-beta2m(o/o) and NK1.1-depleted BALB/c-NK1.1+ mice developed a progressive, nonhealing disease that was indistinguishable from wild-type mice. Upon infection, early induction of IL-4 mRNA in the lymph node was not affected in BALB/c-beta2m(o/o) and in NK1.1-depleted BALB/c-NK1.1+ mice, but was abrogated by injection of a CD4-depleting Ab. These data suggest that, in the lymph node, MHC class I-dependent CD4+NK1.1+ T cells do not play a major role in the generation of Th2 responses against L. major. To investigate whether the inability of NK1.1+ T cells to induce IL-4 production in the lymph node was specific to L. major Ag, mice were challenged with low doses of anti-CD3 Ab s.c. in the footpad. In contrast to the spleen, normal levels of IL-4 mRNA were expressed in the lymph nodes of BALB/c-beta2m(o/o) mice. Thus, the MHC class I-dependent CD4+NK1.1+ cell population that gives a rapid IL-4 response in the spleen appears not to contribute significantly to early induced IL-4 responses in the popliteal lymph nodes.
脾脏CD4⁺NK1.1⁺ T细胞已被证明在静脉注射抗CD3抗体90分钟后会分泌大量且短暂的IL-4 mRNA,这表明这种新型T细胞亚群可能通过在免疫反应开始时快速提供IL-4来诱导脾脏中的Th2反应。已证明β2-微球蛋白缺陷(β2m⁰/⁰)小鼠体内NK1.1⁺ T细胞数量大幅减少,并且在响应抗CD3时快速诱导IL-4 mRNA的能力严重受损,这表明这些细胞依赖MHC I类分子。为了研究CD4⁺NK1.1⁺ T细胞在针对硕大利什曼原虫的Th2反应诱导中的作用,我们剖析了BALB/c-β2m⁰/⁰小鼠和经抗NK1.1处理的表达NK1.1标记的同基因BALB/c小鼠(BALB/c-NK1.1⁺)针对该寄生虫引发的免疫反应的起始和结果。BALB/c-β2m⁰/⁰小鼠和NK1.1缺失的BALB/c-NK1.1⁺小鼠均发展为进行性、不愈合的疾病,与野生型小鼠无异。感染后,BALB/c-β2m⁰/⁰小鼠和NK1.1缺失的BALB/c-NK1.1⁺小鼠淋巴结中IL-4 mRNA的早期诱导不受影响,但注射CD4耗竭抗体可消除这种诱导。这些数据表明,在淋巴结中,依赖MHC I类分子的CD4⁺NK1.1⁺ T细胞在针对硕大利什曼原虫的Th2反应产生中不起主要作用。为了研究NK1.1⁺ T细胞在淋巴结中无法诱导IL-4产生是否特定于硕大利什曼原虫抗原,小鼠在足垫皮下注射低剂量抗CD3抗体进行攻击。与脾脏不同,但BALB/c-β2m⁰/⁰小鼠淋巴结中IL-4 mRNA表达水平正常。因此,在脾脏中产生快速IL-4反应的依赖MHC I类分子的CD4⁺NK1.1⁺细胞群体似乎对腘窝淋巴结中早期诱导的IL-4反应贡献不大。
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