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免疫反应的遗传控制:特定氨基酸序列抗原被Ir-1基因系统识别的能力。

Genetic control of the immune response: ability of antigens of defined amino acid sequence to be recognized by the Ir-1 gene system.

作者信息

Seaver S S, Brown A, Hämmerling G, McDevitt H O

出版信息

Eur J Immunol. 1976 Jul;6(7):502-7. doi: 10.1002/eji.1830060711.

Abstract

Mice were injected with a series of (T,G)-A--L[poly (L Tyr, L Glu)-poly DL Ala)--poly (L Lys)]-like compounds with side chains of homogeneous sequences: T-A--L, GT-A--L, GGT-A--L, and TG-A--L. T-A--L was not immunogenic. However, T-A--L was able to bind antibodies to (T, G)-A--L 509, and this binding could not be blocked by A--L. When complexed with bovine serum albumin, T-A--L, was immunogenic in both responder and nonresponder strains of mice. GT-A--L and GGT-A--L were both immunogenic and elicited the characteristic responder-nonresponder difference induced by (T,G)-A--L. TG-A--L was also immunogenic, but there was considerable overlap in the response of responder and nonresponder strains. On the average, responder mouse serum had a slightly higher antigen-binding capacity than nonresponder mouse serum. In contrast to antibodies against GGT-A--L, antibodies against TG-A--L bound heterologous antigens poorly. These data, along with the results of other investigators, are consistent with the hypothesis that there are multiple Ir- 1 genes which recognize different sequences. The specificity of the Ir- 1 genes is extraordinary. The polypeptides TG-A--L, TGTG-A--L and GTTG-A--L do not appear to be recognized by these genes.

摘要

给小鼠注射了一系列具有均一序列侧链的(T,G)-A--L[聚(L-酪氨酸,L-谷氨酸)-聚-DL-丙氨酸)--聚(L-赖氨酸)]样化合物:T-A--L、GT-A--L、GGT-A--L和TG-A--L。T-A--L没有免疫原性。然而,T-A--L能够结合针对(T,G)-A--L 509的抗体,并且这种结合不能被A--L阻断。当与牛血清白蛋白复合时,T-A--L在小鼠的应答和不应答品系中均具有免疫原性。GT-A--L和GGT-A--L都具有免疫原性,并引发了由(T,G)-A--L诱导的特征性应答者-非应答者差异。TG-A--L也具有免疫原性,但应答和不应答品系的反应有相当大的重叠。平均而言,应答小鼠血清的抗原结合能力略高于非应答小鼠血清。与针对GGT-A--L的抗体相比,针对TG-A--L的抗体与异源抗原的结合较差。这些数据,连同其他研究者的结果,与存在多个识别不同序列的Ir-1基因的假设一致。Ir-1基因的特异性非常高。多肽TG-A--L、TGTG-A--L和GTTG-A--L似乎不被这些基因识别。

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