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白内障柴田(CTS)小鼠的免疫缺陷。II. 体内T细胞介导的免疫反应受损。

Immune deficiency of cataract Shionogi (CTS) mouse. II. Impaired in vivo T cell-mediated immune response.

作者信息

Yagi H, Nagata M, Takeuchi M, Watanabe A, Arimura A, Hashimoto S, Makino S, Harada M

机构信息

Shionogi Research Laboratories, Shionogi & Co., Ltd., Osaka, Japan.

出版信息

Immunol Invest. 1990 Oct-Dec;19(5-6):493-505. doi: 10.3109/08820139009052975.

Abstract

Our previous study demonstrated that cataract Shionogi (CTS) mice, an inbred strain related to non-obese diabetic (NOD) mice, are T lymphocytopenic and that their T cell-mediated in vitro reactions, such as proliferative responses of spleen cells to T cell mitogens and alloantigens or production of IL 2 and IL 2 receptors after stimulation of spleen cells with Con A, are greatly reduced. To confirm these in vitro characteristics, in vivo immune responses of CTS mice to T-dependent and T-independent antigens were compared with those of some reference strains including NOD mice. Antibody responses of CTS mice after one injection of a high dose (10(8)) or one or two injections of a low dose (10(5)) of sheep red blood cells (SRBC) were markedly lower than those of the reference strains. The decrease was particularly striking in the IgM antibody production at primary response to both high and low doses, and the IgG antibody production at the secondary response to low dose. Similar lower antibody production was observed in CTS mice against bovine serum albumin (BSA). Little production of IgE antibody was observed from 1 through 3 weeks after an injection of BSA plus Bordetella pertussis. IgG1 response was observed at high incidence but lower in titer than those in the reference strains. Unexpectedly, in spite of the poor antibody production to BSA, potent systemic sensitization for anaphylactic shock was easily established; incidence of lethal shock being comparable with those in the reference strains. This suggests that CTS mice are highly susceptible to the effector phase of active anaphylactic shock. Cell-mediated immunity was also impaired. Delayed type of hypersensitivity to SRBC was low, and the rejection of the skin graft from NOD mouse did not occur. In contrast to the reduced T cell-mediated responses, no difference was found between CTS and reference strains with regard to the antibody production to LPS, a T-independent antigen. These in vivo findings are consistent with the previous in vitro study.

摘要

我们之前的研究表明,白内障柴田(CTS)小鼠是一种与非肥胖糖尿病(NOD)小鼠相关的近交系,其T淋巴细胞减少,并且它们的T细胞介导的体外反应,如脾细胞对T细胞有丝分裂原和同种抗原的增殖反应,或用刀豆蛋白A刺激脾细胞后白细胞介素2(IL-2)和IL-2受体的产生,都大大降低。为了证实这些体外特征,将CTS小鼠对T细胞依赖性和T细胞非依赖性抗原的体内免疫反应与包括NOD小鼠在内的一些参考品系的反应进行了比较。CTS小鼠在单次注射高剂量(10⁸)或一到两次注射低剂量(10⁵)绵羊红细胞(SRBC)后的抗体反应明显低于参考品系。这种降低在对高剂量和低剂量的初次反应中的IgM抗体产生以及对低剂量的二次反应中的IgG抗体产生中尤为显著。在CTS小鼠中针对牛血清白蛋白(BSA)也观察到类似的较低抗体产生。在注射BSA加百日咳博德特氏菌后的1至3周内,几乎没有观察到IgE抗体产生。观察到IgG1反应发生率较高,但滴度低于参考品系。出乎意料的是,尽管对BSA的抗体产生较差,但对过敏性休克的强效全身致敏很容易建立;致死性休克的发生率与参考品系相当。这表明CTS小鼠对主动过敏性休克的效应阶段高度敏感。细胞介导的免疫也受损。对SRBC的迟发型超敏反应较低,并且未发生来自NOD小鼠的皮肤移植物排斥。与T细胞介导的反应降低相反,在CTS小鼠和参考品系之间,对T细胞非依赖性抗原脂多糖(LPS)的抗体产生没有差异。这些体内研究结果与之前的体外研究一致。

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