Nagarkatti P S, Sweeney G D, Gauldie J, Clark D A
Toxicol Appl Pharmacol. 1984 Jan;72(1):169-76. doi: 10.1016/0041-008x(84)90261-8.
Susceptibility of mice to a variety of toxic effects of 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) is genetically determined by the Ah locus. To determine if immunotoxicity following TCDD exposure was also regulated by the Ah locus, we tested the ability of low dose TCDD (4 ng/kg) to suppress the generation of allospecific cytotoxic T cells (CTL) by lymphocytes from "susceptible" C57B1/6, and "resistant" DBA/2, and from C57B1/6XDBA/2J F1 hybrid mice in vitro. To determine if TCDD acted directly on the "susceptible" lymphoid cells, the immune response of C57B1/6 leads to DBA/2 and DBA leads to C57B1/6 bone marrow chimeras was also measured. C57B1/6 and F1 mice proved susceptible to suppression consistent with the dominant effect of Ah. Susceptibility to suppression in chimeric mice, however, was determined by the Ah genotype of the host and not by the genotype of the grafted lymphomyeloid cells. Mixing experiments demonstrated that suppression of CTL generation by TCDD was due to suppressor T cells. The frequency of CTL precursors was not affected by TCDD. These results are consistent with the idea that TCDD acts by an Ah locus-dependent mechanism to indirectly promote development of suppressor T cells that block the generation of CTL from their precursors.
小鼠对2,3,7,8-四氯二苯并对二恶英(TCDD)多种毒性作用的易感性由Ah基因座遗传决定。为了确定TCDD暴露后的免疫毒性是否也受Ah基因座调控,我们在体外测试了低剂量TCDD(4 ng/kg)对来自“易感”的C57B1/6、“抗性”的DBA/2以及C57B1/6×DBA/2J F1杂交小鼠的淋巴细胞产生同种特异性细胞毒性T细胞(CTL)的抑制能力。为了确定TCDD是否直接作用于“易感”淋巴细胞,还检测了C57B1/6→DBA/2和DBA→C57B1/6骨髓嵌合体的免疫反应。C57B1/6和F1小鼠被证明对抑制敏感,这与Ah的显性效应一致。然而,嵌合小鼠对抑制的易感性由宿主的Ah基因型决定,而非移植的淋巴髓样细胞的基因型。混合实验表明,TCDD对CTL产生的抑制作用是由抑制性T细胞引起的。TCDD不影响CTL前体的频率。这些结果与以下观点一致,即TCDD通过Ah基因座依赖性机制间接促进抑制性T细胞的发育,这些抑制性T细胞阻止CTL前体产生CTL。
