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“决定簇选择”和“T细胞库中的漏洞”对T细胞反应的相对贡献。

Relative contribution of "determinant selection" and "holes in the T-cell repertoire" to T-cell responses.

作者信息

Schaeffer E B, Sette A, Johnson D L, Bekoff M C, Smith J A, Grey H M, Buus S

机构信息

Department of Medicine, National Jewish Center for Immunology and Respiratory Medicine, Denver, CO 80206.

出版信息

Proc Natl Acad Sci U S A. 1989 Jun;86(12):4649-53. doi: 10.1073/pnas.86.12.4649.

Abstract

Using BALB/c and CBA/J mice, the I-region associated (Ia) binding capacity and T-cell immunogenicity of a panel of 14 overlapping peptides that span the entire sequence of the protein staphylococcal nuclease (Nase) was examined to evaluate major histocompatibility gene complex (MHC) control of T-cell responses. Ia binding and Ia-restricted T-cell immunogenicity could be determined for a total of 54 peptide-MHC combinations. Only 30% of the 54 instances examined involved detectable Ia binding, but they represented almost all (12 of 13) of the immune responses found. However, binding to Ia was not sufficient to ensure T-cell immunogenicity, since only 70% of the binding events were productive--i.e., were associated with an immune response. Thus, Ia molecules have the expected characteristics of a highly permissive capacity for antigen interaction that allows them to function as restriction elements for a large universe of antigens. On the other hand, since the Ia molecules cannot distinguish between self and non-self, not all antigen-Ia interactions would be permitted to elicit a T-cell response. It appears that both Ia binding ("determinant selection") and T-cell repertoire act in concert to define the immune response status of an individual toward any particular T-cell epitope.

摘要

利用BALB/c和CBA/J小鼠,检测了一组覆盖葡萄球菌核酸酶(Nase)蛋白整个序列的14个重叠肽段的I区相关(Ia)结合能力和T细胞免疫原性,以评估主要组织相容性基因复合体(MHC)对T细胞应答的控制作用。总共可确定54种肽-MHC组合的Ia结合和Ia限制的T细胞免疫原性。在所检测的54个实例中,只有30%涉及可检测到的Ia结合,但它们几乎代表了所有(13个中的12个)发现的免疫应答。然而,与Ia的结合不足以确保T细胞免疫原性,因为只有70%的结合事件是有成效的——即与免疫应答相关。因此,Ia分子具有预期的高度宽松的抗原相互作用能力特征,使其能够作为大量抗原的限制元件发挥作用。另一方面,由于Ia分子无法区分自身和非自身,并非所有抗原-Ia相互作用都能引发T细胞应答。看来,Ia结合(“决定簇选择”)和T细胞库共同作用,以确定个体对任何特定T细胞表位的免疫应答状态。

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