Section of Allergy and Clinical Immunology, Department of Internal Medicine, Yale University School of Medicine, New Haven, CT, USA.
Scand J Immunol. 2011 May;73(5):465-77. doi: 10.1111/j.1365-3083.2011.02522.x.
Prior studies of classical 24 h responses in TNP-Cl (picryl chloride) allergic contact sensitivity (CS), showed mediation by Th1 cells in CBA mice, and established that 24 h elicitation of responses requires an early 2 h CS-initiating component dependent on iNKT cells, IL-4 and B-1 B cells. Here, we studied the other form of cytotoxic T cell (Tc1) CS in DNFB sensitized BALB/c mice and determined that similar CS-initiation also is required. We systematically tested each step of the initiation pathway in this model. Thus, DNFB Tc1 CS was significantly impaired in iNKT cell deficient CD1d(-/-) and Jα18(-/-) mice, IL4Rα(-/-) and STAT-6(-/-) mice, and also in pan B-cell deficient JH(-/-) mice. Further, the Tc1 DNFB CS-initiating component, like Th1 response to TNP-Cl, was elicited by only 1-day after immunization, due to B-1 cells. In summary, we show that CS-Initiation also is required in Tc1 CS. Further, we have newly determined regulatory support of both the early and late components of DNFB induced Tc1 CS by iNKT cells and γδ-T cells. In summary, both iNKT cells and assisting γδ-T cells are involved in initiating and effector phases of DNFB induced CS.
先前对 TNP-Cl(苦味酸氯)过敏接触敏感性(CS)的经典 24 小时反应的研究表明,CBA 小鼠中的 Th1 细胞介导了该反应,并证实了 24 小时反应的诱导需要早期 2 小时的 CS 起始成分,该成分依赖于 iNKT 细胞、IL-4 和 B-1 B 细胞。在这里,我们研究了二硝基氟苯(DNFB)致敏 BALB/c 小鼠中的另一种细胞毒性 T 细胞(Tc1)CS,并确定类似的 CS 起始也需要。我们系统地测试了该模型中起始途径的每个步骤。因此,iNKT 细胞缺陷型 CD1d(-/-)和 Jα18(-/-)小鼠、IL4Rα(-/-)和 STAT-6(-/-)小鼠以及全 B 细胞缺陷型 JH(-/-)小鼠中的 DNFB Tc1 CS 明显受损。此外,与 TNP-Cl 反应的 Th1 反应一样,Tc1 DNFB CS 起始成分仅在免疫后 1 天即可被引发,这是由于 B-1 细胞所致。总之,我们表明 Tc1 CS 也需要 CS 起始。此外,我们还新确定了 iNKT 细胞和 γδ-T 细胞对 DNFB 诱导的 Tc1 CS 的早期和晚期成分的调节支持。总之,iNKT 细胞和辅助 γδ-T 细胞都参与了 DNFB 诱导的 CS 的起始和效应阶段。
