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淋巴细胞对蛋白质抗原的特异性。V. 细胞色素c特异性T细胞激活的构象依赖性

Lymphocyte specificity to protein antigens. V. Conformational dependence of activation of cytochrome c-specific T cells.

作者信息

Buchmüller Y, Corradin G

出版信息

Eur J Immunol. 1982 May;12(5):412-6. doi: 10.1002/eji.1830120510.

Abstract

Variations in the immunogenic and antigenic properties of native and denatured forms of cytochrome c were observed depending on the strain of mouse tested. In C57BL/6 and (C57BL/6 X DBA/2)F1 (BDF1) mice, priming with either native or denatured cytochrome c (apocytochrome c) gave rise to T cell blasts responding in a similar fashion to the two forms of the antigen and to different peptides derived from CNBr cleavage of the protein when tested for proliferation in the presence of C57BL/6 or BDF1 accessory cells. A different pattern of proliferation was observed when apocytochrome c-specific DBA/2 or BDF1 T cell blasts were tested with DBA/2 accessory cells. In this case, no response was obtained to heme peptide 1-65. This was not due to an inability of DBA/2 macrophages to process and present heme peptide 1-65, as they were able to present this antigen to native cytochrome c-specific BDF1 T cell blasts. Thus, it seems that different sets of clones are generated upon priming BDF1 mice with denatured cytochrome c which are able to recognize different sets of peptides depending on the nature of the accessory cells. The results obtained are consistent with the hypothesis that degradation and presentation of native and denatured cytochrome c by macrophages is dependent on the three-dimensional conformation of the protein.

摘要

根据所测试小鼠的品系,观察到细胞色素c天然形式和变性形式的免疫原性和抗原性存在差异。在C57BL/6和(C57BL/6×DBA/2)F1(BDF1)小鼠中,用天然或变性细胞色素c(脱辅基细胞色素c)进行初次免疫,会产生T细胞母细胞,当在C57BL/6或BDF1辅助细胞存在的情况下测试增殖时,这些T细胞母细胞对两种形式的抗原以及该蛋白质经溴化氰裂解产生的不同肽段的反应方式相似。当用DBA/2辅助细胞测试脱辅基细胞色素c特异性的DBA/2或BDF1 T细胞母细胞时,观察到了不同的增殖模式。在这种情况下,对血红素肽1 - 65没有反应。这并非由于DBA/2巨噬细胞无法处理和呈递血红素肽1 - 65,因为它们能够将该抗原呈递给天然细胞色素c特异性的BDF1 T细胞母细胞。因此,在用变性细胞色素c对BDF1小鼠进行初次免疫时,似乎会产生不同的克隆集,这些克隆集能够根据辅助细胞的性质识别不同的肽段集。所获得的结果与以下假设一致,即巨噬细胞对天然和变性细胞色素c的降解和呈递取决于蛋白质的三维构象。

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