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特异性免疫抑制的遗传控制。IV. 环磷酰胺诱导BALB/c小鼠对随机共聚物L-谷氨酸50-L-酪氨酸50的反应性。

Genetic control of specific immune suppression. IV. Responsiveness to the random copolymer L-glutamic acid50-L-tyrosine50 induced in BALB/c mice by cyclophosphamide.

作者信息

Debré P, Waltenbaugh C, Dorf M E, Benacerraf B

出版信息

J Exp Med. 1976 Jul 1;144(1):277-81. doi: 10.1084/jem.144.1.277.

Abstract

Previous reports from our laboratory have demonstrated the stimulation of specific suppressor T cells in genetic nonresponder mice after immunization with the terpolymer of L- glutamic acid, L-alanine, and L-tyrosine (GAT) (1,2) and with the copolymer of L-glutamic acid and L-tyrosine (GT) (3-5). These findings raise two important questions: (a) do the specific suppressor T cells inhibit an antibody response which would otherwise develop in nonresponder mice; and, (b) can specific helper T cells inhibit an antibody response which would otherwise develop in nonresponder mice; and, (b) can specific helper T-cell activity be detected in these animals. Responsiveness appears to be completely dominant over suppression in (responder x suppressor)F(1) hybrids, therefore, we have been unable to detect suppressor cells in these hybrids after conventional immunization with GAT (2). However , using special conditions of antigen administration, GAT helper activity could be demonstrated in nonresponder DBA/1 ("suppressor") mice. Thus, GAT-specific helper activity was not detected in these nonresponder animals after immunization with GAT irrespective of the adjuvant used, but could be stimulated by macrophage-bound GAT or by GAT complexed with methylated bovine serum albumin GAT-MBSA (6). In the current report we have taken advantage of the fact that suppressor T-cell activity is more sensitive to cyclophosphamide treatment than T-cell helper activity (7) to demonstrate the presence of GT-specific helper activity in "nonresponder" BALB/c mice. We describe: (a) the dose of cyclophosphamide and conditions of treatment which inhibits the well-documented stimulation of specific suppressor T cells in BALB/c mice injected with GT previous to immunization with GT-MBSA, and (b) the ability of cyclophosphamide to permit the development of primary PFC responses to GT in these "nonresponder" mice. These cyclophosphamide-induced responses are not characterized by the high levels of antibody detected in genetic responder animals.

摘要

我们实验室之前的报告已经证明,在用L-谷氨酸、L-丙氨酸和L-酪氨酸的三元共聚物(GAT)(1,2)以及L-谷氨酸和L-酪氨酸的共聚物(GT)(3-5)免疫后,基因无反应小鼠中特定抑制性T细胞受到刺激。这些发现提出了两个重要问题:(a)特定抑制性T细胞是否会抑制无反应小鼠中原本会产生的抗体反应;以及(b)特定辅助性T细胞是否能抑制无反应小鼠中原本会产生的抗体反应;以及(b)在这些动物中能否检测到特定辅助性T细胞活性。在(反应者×抑制者)F1杂种中,反应性似乎完全显性于抑制作用,因此,在用GAT进行常规免疫后,我们无法在这些杂种中检测到抑制性细胞(2)。然而,使用特殊的抗原给药条件,可以在无反应的DBA/1(“抑制者”)小鼠中证明GAT辅助活性。因此,在用GAT免疫后,无论使用何种佐剂,在这些无反应动物中均未检测到GAT特异性辅助活性,但可以通过巨噬细胞结合的GAT或与甲基化牛血清白蛋白GAT-MBSA复合的GAT来刺激(6)。在本报告中,我们利用抑制性T细胞活性比T细胞辅助活性对环磷酰胺治疗更敏感这一事实(7),来证明“无反应”BALB/c小鼠中存在GT特异性辅助活性。我们描述了:(a)环磷酰胺的剂量和治疗条件,其抑制在用GT-MBSA免疫前注射GT的BALB/c小鼠中已充分记录的特定抑制性T细胞的刺激,以及(b)环磷酰胺使这些“无反应”小鼠中对GT产生原发性PFC反应的能力。这些环磷酰胺诱导的反应并不以基因反应动物中检测到的高水平抗体为特征。

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