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Enhanced positive selection of a transgenic TCR by a restriction element that does not permit negative selection

机译:通过不允许负选择的限制元件增强了转基因TCR的正选择

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摘要

Very little is known about the conformational properties of the MHC molecules that are able to signal positive selection of a given TCR. To try to understand these parameters and to determine whether these requirements are shared with interactions during negative selection and antigen recognition, we have studied selection and antigen recognition of a transgenic TCR (specific for lymphocytic choriomeningitls virus glycoprotein and H-2Db) in the context of two Db mutants, H-2bm13 and H-2bm14. The data showed that the transgenic TCR was not positively selected by the H-2bm14 haplotype but, interestingly, enhanced positive selection was seen in H-2bm13 mice. The transgenic TCR could not be negatively selected In H-2bm13animals persistently infected with the virus (neonatal virus carrier mice), nor could the transgenic TCR be activated by H-2bm13 infected cells in vivo or in vitro. These experiments show that although a TCR may be selected by a mutant MHC molecule, the corresponding viral antigen cannot be recognized in the context of the mutant MHC molecule, as Judged by both negative selection and T cell reactivity in vivo and in vitro. The ‘enhanced' positive selection occurring in the context of Dbm13 suggests that a different conformation of the MHC molecule is able to select the same TCR and also that various TCR-ligand avidities may permit positive selection
机译:关于MHC分子的构象特性知之甚少,这些构象特性能够表示对给定TCR的阳性选择。为了试图理解这些参数并确定在负选择和抗原识别期间相互作用是否需要这些要求,我们研究了转基因TCR(对淋巴细胞脉络膜脑膜炎病毒糖蛋白和H-2Db特异)的选择和抗原识别。两个Db突变体H-2bm13和H-2bm14。数据显示,H-2bm14单倍型未对转基因TCR进行阳性选择,但有趣的是,在H-2bm13小鼠中看到了增强的阳性选择。在持续感染该病毒的H-2bm13动物(新生病毒载体小鼠)中,不能阴性选择转基因TCR,也不能在体内或体外通过H-2bm13感染的细胞激活转基因TCR。这些实验表明,尽管TCR可以由突变的MHC分子选择,但是相应的病毒抗原不能在突变的MHC分子的背景下被识别,如通过体内和体外的阴性选择和T细胞反应性判断。在Dbm13上下文中发生的“增强”阳性选择表明,MHC分子的不同构象能够选择相同的TCR,而且各种TCR配体亲和力可能允许阳性选择

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