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H-43a和H-43b小鼠中细胞毒性T淋巴细胞对次要H-43同种抗原的反应。抗H-43b和抗H-43a细胞毒性T淋巴细胞活性均仅在相同的H-2Kb限制元件背景下产生。

Cytotoxic T lymphocyte responses to minor H-43 alloantigens in H-43a and H-43b mice. Both anti-H-43b and anti-H-43a CTL activities are generated exclusively in the context of the same H-2Kb restriction element.

作者信息

Ishikawa H, Kusakabe A, Hayakawa J, Hino T

机构信息

Department of Microbiology, Keio University School of Medicine, Tokyo, Japan.

出版信息

J Immunol. 1988 Nov 1;141(9):2918-23.

PMID:3139769
Abstract

We have previously demonstrated that anti-H-43a CTL response of H-43b responder mice was exclusively restricted by self H-2Kb (Kb) but not by the other nine self MHC class I alleles from independent origins, i.e., Kbml,d,k,s and Db,d,k,q,s. In the present study, we verified that Kf,q,r and Df,r alleles could also not serve as restricting class I elements in the CTL response to H-43a alloantigen. Another notable observation made in the earlier study was the fact that, in H-43 incompatibility of the alternative combination, H-43a mice were incapable of generating CTL activity against H-43b alloantigen. However, by means of employing new in vivo immunization procedures, we discovered that some but not all genetically identical H-43a responder mice could mount anti-H-43b CTL response restricted by self Kb. Again, no anti-H-43b CTL activity could be generated in the context of self Kk, Kj, Db or Dk molecules. Although the number of class I alleles we examined is still limited, these results indicate that antigenic fragments derived from the processed H-43a and H-43b alloantigens possess an indistinguishable epitope (agretope), and that such agretope either interacts only with the privileged Kb molecules or allows to bestow the immunogenic conformation of allodeterminants on the fragments solely in the context of the restricting Kb element.

摘要

我们之前已经证明,H-43b反应小鼠的抗H-43a细胞毒性T淋巴细胞(CTL)反应仅受自身H-2Kb(Kb)限制,而不受来自独立起源的其他九个自身MHC I类等位基因限制,即Kbml、d、k、s和Db、d、k、q、s。在本研究中,我们证实Kf、q、r和Df、r等位基因在针对H-43a同种异体抗原的CTL反应中也不能作为限制性I类元件。早期研究中另一个值得注意的观察结果是,在替代组合的H-43不相容性中,H-43a小鼠无法产生针对H-43b同种异体抗原的CTL活性。然而,通过采用新的体内免疫程序,我们发现一些但并非所有基因相同的H-43a反应小鼠能够产生受自身Kb限制的抗H-43b CTL反应。同样,在自身Kk、Kj、Db或Dk分子的情况下,无法产生抗H-43b CTL活性。尽管我们检测的I类等位基因数量仍然有限,但这些结果表明,来自加工后的H-43a和H-43b同种异体抗原的抗原片段具有难以区分的表位(抗原决定基),并且这种抗原决定基要么仅与特权Kb分子相互作用,要么仅在限制性Kb元件的背景下允许赋予片段上同种异体决定簇的免疫原性构象。

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