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The in vitro induction of immunological tolerance in the B lymphocyte by oligovalent thymus-dependent antigens

机译:低价胸腺依赖性抗原体外诱导B淋巴细胞免疫耐受

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摘要

B-cell tolerance has been induced by oligovalent thymus-dependent antigens in an entirely in vitro system. Dissociated spleen cells from congenitally athymic (nuu) mice were preincubated for 24 h with 0.1 -- 1 mg/ml of either fowl gamma globulin (FGG) of DNP-human gamma globulin (DNP-HGG). After washing, the cells were tested for the ability to mount in vitro, thymus-independent responses against FGG and DNP. A state of specific responsiveness to either FGG or DNP was thus demonstrated. Features of this wholly in vitro system that paralleled previous findings on the in vivo induction of B-cell tolerance in nuu mice were the kinetics, 24 h being required for tolerance induction in either case, the abrogation of tolerance induction by the presence of POL both in vivo and in vitro, and finally the observation that in neither case was there a requirement for the antigens to be deaggregated. It was shown that DNP-(Fab) 2 fragments prepared from HGG induced DNP-specific tolerance indicating that the Fc piece was not required for tolerance induction in this in vitro system. DNP-bovine serum albumin was less effective than DNP-HGG or DNP-(Fab)2. Preincubation with subtoxic concentrations of DNP-lysine of DNP-epsilon- capric acid had only a marginal effect on DNP responsiveness. Since nuu mice, lacking in detectable T-cell function, were used as spleen cell donors, this work provides further evidence that B-cell tolerance to thymus-dependent antigens can be induced without the participation of T cells. It is suggested that B-cell tolerance to thymus-dependent antigens occurs when the antigen in a sufficient concentration and over a sufficient period of time has direct access to the B cell. This contact with antigen must be in the absence of an additional influence provided either by adjuvants like endotoxin or POL, or by activated macrophages, which may be stimulated by activated T cells; otherwise not tolerance but B-cell activation will occur.
机译:在完全体外的系统中,寡聚胸腺依赖性抗原已诱导了B细胞耐受性。将先天性无胸腺(nu / nu)小鼠的脾脏细胞与0.1-1 mg / ml的DNP-人γ球蛋白(DNP-HGG)的家禽γ球蛋白(FGG)一起预孵育24 h。清洗后,测试细胞针对FGG和DNP进行体外,胸腺非依赖性应答的能力。因此证明了对FGG或DNP的特异性应答状态。这种完全体外的系统的特征与先前在nu / nu小鼠体内诱导B细胞耐受性的发现相近,其动力学是动力学,在任何情况下都需要24 h诱导耐受性,由于存在n可以消除耐受性诱导体内和体外的POL,最后观察到在两种情况下都不需要分解抗原。从HGG制备的DNP-(Fab)2片段显示出诱导的DNP特异性耐受性,表明在该体外系统中不需要Fc片段来诱导耐受性。 DNP-牛血清白蛋白的疗效不及DNP-HGG或DNP-(Fab)2。用亚毒性浓度的DNP-ε-癸酸DNP-赖氨酸进行预温育仅对DNP反应性产生边际影响。由于nu / nu小鼠缺乏可检测的T细胞功能,被用作脾细胞供体,因此这项工作提供了进一步的证据,表明可以在没有T细胞参与的情况下诱导对胸腺依赖性抗原的B细胞耐受。提示当抗原以足够的浓度并在足够的时间段内直接进入B细胞时,就会发生对胸腺依赖性抗原的B细胞耐受。与抗原的这种接触必须没有内毒素或POL等佐剂或活化巨噬细胞提供的其他影响,活化巨噬细胞可能会被活化T细胞刺激。否则不能耐受,但会发生B细胞活化。

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