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通过哺乳接触蛋白质抗原的小鼠缺乏T细胞耐受性。

Lack of T cell tolerance in mice exposed to a protein antigen through lactation.

作者信息

Ryelandt M, De Wit D, Van Mechelen M, Vansanten G, Urbain J, Leo O

机构信息

Laboratoire de Physiologie Animale, Université Libre de Bruxelles, Rhode-Saint-Genèse, Belgium.

出版信息

Cell Immunol. 1995 Apr 15;162(1):89-96. doi: 10.1006/cimm.1995.1055.

Abstract

Offspring of mother mice treated immediately after delivery with deaggregated human gamma-globulins (dHGG) are unable to produce HGG-specific antibodies when challenged with immunogenic forms of HGG (HGG/CFA) in adulthood. Despite a defective antibody response, animals rendered tolerant to HGG as neonates retain tolerogen-specific T cells able to proliferate and secrete lymphokines. The pattern of IL-2 and IL-4 secretion by T cells isolated from tolerant animals could not be distinguished from the corresponding cells in control mice, suggesting that neonatal exposure to dHGG did not affect T cell reactivity or Th1/Th2 in vivo balance. Moreover, immunization of tolerant animals with haptenated HGG confirmed the presence of tolerogen-specific helper T cells in vivo. Functional T cell depletion by anti-CD3 mAbs during lactation failed to modify induction of B cell tolerance, suggesting that T cells are neither affected nor required to induce the selective tolerance status observed in this model. Based on the finding that antigen-presenting cell functions in secondary organs (spleen, peritoneal cavity) are a late acquisition during ontogeny and reach adult-like levels at weaning, we propose that most soluble proteins elude T cell recognition during lactation due to defective antigen presentation.

摘要

产后立即用解聚的人γ-球蛋白(dHGG)处理的母鼠所生后代,成年后用免疫原性形式的HGG(HGG/CFA)攻击时,无法产生HGG特异性抗体。尽管抗体反应存在缺陷,但新生期对HGG产生耐受的动物保留了能够增殖和分泌淋巴因子的耐受原特异性T细胞。从耐受动物分离的T细胞分泌IL-2和IL-4的模式与对照小鼠的相应细胞无法区分,这表明新生期接触dHGG在体内并未影响T细胞反应性或Th1/Th2平衡。此外,用半抗原化HGG对耐受动物进行免疫证实了体内存在耐受原特异性辅助性T细胞。哺乳期用抗CD3单克隆抗体进行功能性T细胞耗竭未能改变B细胞耐受的诱导,这表明T细胞既未受到影响,也不是诱导该模型中观察到的选择性耐受状态所必需的。基于次级器官(脾脏、腹腔)中的抗原呈递细胞功能在个体发育过程中获得较晚且在断奶时达到成年水平这一发现,我们提出,由于抗原呈递存在缺陷,大多数可溶性蛋白质在哺乳期逃避了T细胞的识别。

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