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白细胞介素-12 p40同二聚体的体内产生及功能

In vivo production and function of IL-12 p40 homodimers.

作者信息

Heinzel F P, Hujer A M, Ahmed F N, Rerko R M

机构信息

Division of Geographic Medicine, Case Western Reserve University School of Medicine, and Veterans Affairs Medical Center, Cleveland, OH 44106, USA.

出版信息

J Immunol. 1997 May 1;158(9):4381-8.

PMID:9127002
Abstract

The bioactivity of IL-12 is mediated by heterodimers of disulfide-linked p35 and p40 protein subunits. Homodimeric p40 competes with heterodimer for binding to the high affinity IL-12R and inhibits IL-12 bioactivity in vitro. However, the production and significance of p40 homodimer as a cytokine antagonist in vivo have not been determined. In these studies, we observed increased amounts of both IL-12 p40 monomer and homodimer in the serum of C57BL/6 mice following injection of 300 microg of Salmonella enteritidis LPS. Homodimer constituted between 20 and 40% of the total circulating p40 in endotoxemic sera, as confirmed by both Sephacryl S-100 gel filtration and p40-specific immunoprecipitation analyses. Similar relative amounts of homodimer and monomer were observed in endotoxemic BALB/c, C57BL/6, IFN-gamma-deficient C57BL/6 mice and C57BL/6 mice previously infected with bacille Calmette-Guérin. To determine whether IL-12 p40 homodimer was capable of antagonizing IL-12-dependent IFN-gamma responses in vivo, we pretreated C57BL/6 mice with purified rIL-12 p40 homodimer before i.p. challenge with endotoxin. Mice treated with 40 to 80 microg of p40 homodimer generated 80 to 82% less circulating IFN-gamma during acute endotoxemia than saline controls (p < 0.01). We conclude that p40 homodimer is produced in vivo, functions as a cytokine antagonist in the context of the mouse model of acute endotoxemia, and may represent a novel form of self-regulating cytokine response.

摘要

白细胞介素-12(IL-12)的生物活性由通过二硫键连接的p35和p40蛋白亚基的异二聚体介导。同二聚体p40与异二聚体竞争结合高亲和力的IL-12受体,并在体外抑制IL-12的生物活性。然而,p40同二聚体作为体内细胞因子拮抗剂的产生及意义尚未确定。在这些研究中,我们观察到给C57BL/6小鼠注射300微克肠炎沙门氏菌脂多糖(LPS)后,血清中IL-12 p40单体和同二聚体的量均增加。通过Sephacryl S-100凝胶过滤和p40特异性免疫沉淀分析证实,同二聚体在内毒素血症血清中占循环p40总量的20%至40%。在内毒素血症的BALB/c、C57BL/6、γ干扰素缺陷型C57BL/6小鼠以及先前感染过卡介苗的C57BL/6小鼠中观察到同二聚体和单体的相对量相似。为了确定IL-12 p40同二聚体在体内是否能够拮抗依赖IL-12的γ干扰素反应,我们在腹腔注射内毒素攻击前,用纯化的重组IL-12 p40同二聚体预处理C57BL/6小鼠。用40至80微克p40同二聚体处理的小鼠在急性内毒素血症期间产生的循环γ干扰素比生理盐水对照组少80%至82%(p<0.01)。我们得出结论,p40同二聚体在体内产生,在急性内毒素血症小鼠模型中作为细胞因子拮抗剂发挥作用,可能代表一种新型的自我调节细胞因子反应形式。

相似文献

1
In vivo production and function of IL-12 p40 homodimers.白细胞介素-12 p40同二聚体的体内产生及功能
J Immunol. 1997 May 1;158(9):4381-8.
2
IFN-gamma-independent production of IL-12 during murine endotoxemia.小鼠内毒素血症期间白细胞介素-12的γ干扰素非依赖性产生
J Immunol. 1996 Nov 15;157(10):4521-8.
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Mouse interleukin-12 (IL-12) p40 homodimer: a potent IL-12 antagonist.小鼠白细胞介素-12(IL-12)p40 同源二聚体:一种有效的 IL-12 拮抗剂。
Eur J Immunol. 1995 Jan;25(1):200-6. doi: 10.1002/eji.1830250133.
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Differential effects of IL-12 receptor blockade with IL-12 p40 homodimer on the induction of CD4+ and CD8+ IFN-gamma-producing cells.IL-12 p40 同二聚体阻断 IL-12 受体对诱导 CD4+ 和 CD8+ 产生 IFN-γ 的细胞的不同作用。
J Immunol. 1997 Jan 15;158(2):643-8.
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Alloantigen-reactive Th1 development in IL-12-deficient mice.白细胞介素-12缺陷小鼠中同种抗原反应性Th1细胞的发育
J Immunol. 1998 Feb 1;160(3):1132-8.
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Endotoxin fails to induce IFN-gamma in endotoxin-tolerant mice: deficiencies in both IL-12 heterodimer production and IL-12 responsiveness.内毒素无法在对内毒素耐受的小鼠中诱导γ干扰素:白细胞介素-12异二聚体生成及白细胞介素-12反应性均存在缺陷。
J Immunol. 1999 Mar 15;162(6):3633-8.
7
Reduced T helper 1 responses in IL-12 p40 transgenic mice.IL-12 p40转基因小鼠中辅助性T细胞1反应降低。
J Immunol. 1998 Jan 15;160(2):588-94.
8
Human IL-12 p40 homodimer binds to the IL-12 receptor but does not mediate biologic activity.人白细胞介素-12 p40 同二聚体与白细胞介素-12 受体结合,但不介导生物学活性。
J Immunol. 1995 Jan 1;154(1):116-27.
9
Analysis of the multiple interactions between IL-12 and the high affinity IL-12 receptor complex.白细胞介素-12与高亲和力白细胞介素-12受体复合物之间多重相互作用的分析。
J Immunol. 1998 Mar 1;160(5):2174-9.
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Interleukin-12 antagonist activity of mouse interleukin-12 p40 homodimer in vitro and in vivo.小鼠白细胞介素-12 p40同二聚体在体外和体内的白细胞介素-12拮抗剂活性
Ann N Y Acad Sci. 1996 Oct 31;795:1-12. doi: 10.1111/j.1749-6632.1996.tb52650.x.

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