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T细胞疫苗接种的最小模型。

A minimal model for T-cell vaccination.

作者信息

Borghans J A, De Boer R J

机构信息

Utrecht University, The Netherlands.

出版信息

Proc Biol Sci. 1995 Feb 22;259(1355):173-8. doi: 10.1098/rspb.1995.0025.

Abstract

We have developed a mathematical model for the regulation of the growth of autoreactive T cells (the T cells responsible for autoimmunity). The model is very simple in that it is based only on the fundamental properties of T cells. However, despite this simplicity, it can account for a variety of phenomena referred to as T-cell vaccination. The purpose of T-cell vaccination is to create resistance to autoimmunity. This can be achieved by injecting either a subpathogenic quantity of autoreactive T cells, or attenuated autoreactive cells, or cells that recognize the autoreactive cells. The results of our model are based on the assumption that the self antigens involved in T-cell vaccination are normally not expressed; thus the autoreactive T lymphocytes are neither activated nor negatively selected. Self tolerance, therefore, corresponds to a 'passive' state. T-cell vaccination induces a transition from this passive state of tolerance to an active state of tolerance. In this state the autoreactive cells are controlled by regulator cells which recognize the autoreactive cells. The model predicts a qualitative difference between vaccination with normal autoreactive cells and vaccination with attenuated autoreactive cells. Normal cells may give rise to a permanent switch to the vaccinated state; attenuated cells, however, can provide only transient protection, which is dose dependent. Preliminary experimental data confirm this prediction. Finally, we propose a speculative explanation for relapsing autoimmune disease.

摘要

我们已经开发出一种用于调节自身反应性T细胞(引发自身免疫的T细胞)生长的数学模型。该模型非常简单,因为它仅基于T细胞的基本特性。然而,尽管简单,它却能解释各种被称为T细胞疫苗接种的现象。T细胞疫苗接种的目的是建立对自身免疫的抵抗力。这可以通过注射亚致病量的自身反应性T细胞、减毒的自身反应性细胞或识别自身反应性细胞的细胞来实现。我们模型的结果基于这样的假设:参与T细胞疫苗接种的自身抗原通常不表达;因此,自身反应性T淋巴细胞既不被激活也不被阴性选择。所以,自身耐受性对应于一种“被动”状态。T细胞疫苗接种诱导从这种被动耐受状态向主动耐受状态转变。在这种状态下,自身反应性细胞由识别自身反应性细胞的调节细胞控制。该模型预测正常自身反应性细胞疫苗接种和减毒自身反应性细胞疫苗接种之间存在质的差异。正常细胞可能导致永久性转变为接种状态;然而,减毒细胞只能提供短暂的保护,且这种保护是剂量依赖性的。初步实验数据证实了这一预测。最后,我们对复发性自身免疫疾病提出了一种推测性解释。

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