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通过等电聚焦分析甲基化牛血清白蛋白对随机和有序合成多肽的基因调控反应的重建。

Reconstitution of genetically regulated responses against random and ordered synthetic polypeptides by methylated bovine serum albumin as analyzed by isoelectric focusing.

作者信息

Cramer M, Schwartz M, Mozes E, Sela M

出版信息

Eur J Immunol. 1976 Sep;6(9):618-23. doi: 10.1002/eji.1830060905.

Abstract

In previous publications it was shown by avidity measurements, cross-reactivity patterns and genetic analyses, that the tetrapeptide T-T-G-G is the immuno-dominant epitope of the synthetic polypeptide (T, G)-A--L. In the present study this close immunological relationship between the random multichain copolymer (T, G)-A--L and the ordered analogue (T-T-G-G)-A--L is extended by two additional criteria. First, the immune response against (T-T-G-G)-A--L in H-2k nonresponder mouse strains can be reconstituted to high antibody levels by complexing this antigen to methylated bovine serum albumin, as was tested earlier for (T,G)-A--L. The antibodies elicited upon reconstitution in both antigenic systems are directed mainly against the same determinant, T-T-G-G. Second, isoelectric focusing analysis of specific antisera developed with radiolabeled antigen revealed restricted 7 S IgG antibody populations in high responder and reconstituted high and low responder mice. The spectra were found to be of similar complexity in the (T,G)-A--L and in the (T-T-G-G)-A--L system. From these data it was concluded that the repertoires of specific B cells to T-T-G-G are very similar in high and low responder strains, and the defect in the H-2k low responder systems should be located at the level of T-B cell cooperation.

摘要

在之前的出版物中,通过亲和力测量、交叉反应模式和基因分析表明,四肽T-T-G-G是合成多肽(T,G)-A--L的免疫显性表位。在本研究中,随机多链共聚物(T,G)-A--L与有序类似物(T-T-G-G)-A--L之间这种紧密的免疫关系通过另外两个标准得到了扩展。第一,正如之前对(T,G)-A--L所测试的那样,通过将该抗原与甲基化牛血清白蛋白复合,H-2k无反应小鼠品系中针对(T-T-G-G)-A--L的免疫反应可以恢复到高抗体水平。在两个抗原系统中重组后引发的抗体主要针对相同的决定簇T-T-G-G。第二,用放射性标记抗原产生的特异性抗血清的等电聚焦分析显示,在高反应性和重组的高反应性及低反应性小鼠中,7S IgG抗体群体有限。发现(T,G)-A--L和(T-T-G-G)-A--L系统中的光谱复杂性相似。从这些数据可以得出结论,高反应性和低反应性品系中针对T-T-G-G的特异性B细胞库非常相似,H-2k低反应性系统中的缺陷应该位于T-B细胞合作水平。

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