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二次抗原刺激期间的辅助共刺激指导口服耐受诱导的质量方面,尤其是在新生儿期。

Adjuvant costimulation during secondary antigen challenge directs qualitative aspects of oral tolerance induction, particularly during the neonatal period.

作者信息

Tobagus Iriani T, Thomas Wayne R, Holt Patrick G

机构信息

Telethon Institute for Child Health Research, and Center for Child Health Research, Faculty of Medicine and Dentistry, University of Western Australia, Perth, Western Australia, Australia.

出版信息

J Immunol. 2004 Feb 15;172(4):2274-85. doi: 10.4049/jimmunol.172.4.2274.

Abstract

In this report we demonstrate that although passive feeding of specific Ag to mice as neonates or adults can induce oral tolerance in both the cellular and humoral arms of the immune response, quantitative and, in particular, qualitative aspects of the tolerance process are determined by the nature of the inflammatory costimuli provided at the time of secondary Ag challenge. Moreover, this dependency upon nonspecific costimulation is more profound in Ag-fed neonates than in their adult counterparts. Thus, administration of Ag in the Th1-selective adjuvant CFA to prefed animals resulted in significant inhibition of IgG2a, IL-2, and IFN-gamma responses, whereas IL-5 responses were increased. In contrast, rechallenge with Ag in the Th2-selective adjuvant aluminum hydroxide resulted in significant inhibition of IgG1, IgE, IL-2, and IL-5 responses, whereas IFN-gamma responses were increased. Additionally, although soluble Ag challenge of prefed adults revealed marginal tolerogenic effects, the same challenge protocol in animals prefed as neonates elicited enhanced Th2-dependent IgG1 production. These results suggest that inflammatory stimulation at the time of Ag challenge is obligatory to trigger oral tolerance mechanisms, particularly in animals fed as neonates and also that the type of adjuvant used at the time of challenge selects for the type of Th cell population to be inhibited.

摘要

在本报告中,我们证明,尽管在新生期或成年期给小鼠被动喂食特定抗原可在免疫应答的细胞和体液分支中诱导口服耐受,但耐受过程的定量,尤其是定性方面,由再次抗原刺激时提供的炎性共刺激的性质决定。此外,这种对非特异性共刺激的依赖性在喂食抗原的新生小鼠中比在成年小鼠中更为显著。因此,给预先喂食过抗原的动物注射Th1选择性佐剂完全弗氏佐剂(CFA)中的抗原,会导致IgG2a、IL-2和IFN-γ应答受到显著抑制,而IL-5应答则增强。相反,用Th2选择性佐剂氢氧化铝再次刺激抗原,会导致IgG1、IgE、IL-2和IL-5应答受到显著抑制,而IFN-γ应答则增强。此外,尽管对预先喂食过抗原的成年动物进行可溶性抗原刺激显示出轻微的致耐受作用,但在新生期预先喂食过抗原的动物中采用相同的刺激方案会引发增强的Th2依赖性IgG1产生。这些结果表明,抗原刺激时的炎性刺激对于触发口服耐受机制是必不可少的,尤其是在新生期喂食过抗原的动物中,而且刺激时使用的佐剂类型决定了被抑制的Th细胞群体的类型。

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