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卵清蛋白肽/Kb复合物向T细胞的内源性生成及呈递。

Endogenous generation and presentation of the ovalbumin peptide/Kb complex to T cells.

作者信息

Shastri N, Gonzalez F

机构信息

Department of Molecular and Cell Biology, University of California, Berkeley 94720.

出版信息

J Immunol. 1993 Apr 1;150(7):2724-36.

PMID:8454852
Abstract

Peptide fragments are displayed on the APC surface by MHC class I molecules as ligands for appropriate TCR. Sequence analysis of MHC-bound peptide mixtures has suggested that naturally processed peptides are defined by their length and by the presence of MHC allele-defined consensus motifs. To define the minimal OVA peptide presented by Kb MHC, and the requirements for generation of endogenous OVA/Kb complex, APC were transfected with OVA cDNA constructs. We show that optimal stimulation of OVA/Kb-specific B3Z T cell hybrid by Kb-APC requires the OVA257-264 peptide (SIINFEKL, SL8) whether added exogenously, or when synthesized endogenously as precursor polypeptides. Thus, all information necessary for expression of the OVA/Kb complex is contained within the Kb octapeptide motif shared by SL8. Unexpectedly, the SL8/Kb or the influenza NP/Db complexes were also generated in APC even when the peptide coding sequences were placed in incorrect translational reading frames. By contrast, identical manipulations of the translational reading frame of the lacZ reporter gene reduced protein synthesis to undetectable levels demonstrating the remarkable efficiency with which endogenous peptide/MHC are generated in and presented by APC to T cells. These characteristics of the endogenous presentation may explain how large numbers of distinct peptide/MHC complexes are displayed on the cell surface and surveyed by TCR.

摘要

肽片段由MHC I类分子作为适当TCR的配体展示在抗原呈递细胞(APC)表面。对与MHC结合的肽混合物进行序列分析表明,天然加工的肽由其长度以及MHC等位基因定义的共有基序的存在来界定。为了确定由Kb MHC呈递的最小OVA肽以及内源性OVA/Kb复合物生成的要求,用OVA cDNA构建体转染APC。我们发现,无论是外源性添加还是作为前体多肽内源性合成时,Kb-APC对OVA/Kb特异性B3Z T细胞杂交体的最佳刺激都需要OVA257-264肽(SIINFEKL,SL8)。因此,OVA/Kb复合物表达所需的所有信息都包含在SL8共有的Kb八肽基序中。出乎意料的是,即使将肽编码序列置于错误的翻译阅读框中,APC中也会生成SL8/Kb或流感NP/Db复合物。相比之下,对lacZ报告基因的翻译阅读框进行相同操作会使蛋白质合成降低到无法检测的水平,这表明APC在细胞内生成并向T细胞呈递内源性肽/MHC的效率非常高。内源性呈递的这些特征可能解释了大量不同的肽/MHC复合物如何展示在细胞表面并由TCR进行监测。

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