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H-2M缺陷小鼠的表型取决于所表达的MHC II类分子。

The phenotype of H-2M-deficient mice is dependent on the MHC class II molecules expressed.

作者信息

Wolf P R, Tourne S, Miyazaki T, Benoist C, Mathis D, Ploegh H L

机构信息

Department of Pathology, Harvard Medical School, Boston 02115, USA.

出版信息

Eur J Immunol. 1998 Sep;28(9):2605-18. doi: 10.1002/(SICI)1521-4141(199809)28:09<2605::AID-IMMU2605>3.0.CO;2-B.

DOI:10.1002/(SICI)1521-4141(199809)28:09<2605::AID-IMMU2605>3.0.CO;2-B
PMID:9754549
Abstract

For a broader view of the role of H-2M as an accessory molecule in antigen presentation, we investigated the degree to which different MHC class II isotypes and alleles depend on H-2M to function in vivo. We generated H-2M-deficient animals expressing Ek/b or Ak molecules in addition to the Ab molecules already present in the mutant strain, and compared the ability of the different MHC class II molecules to present antigen at the cell surface for recognition by T cells, and contribute to positive selection of CD4+ T cells in the thymus. Biochemical analyses were performed to assess MHC class II maturation, and to determine the peptide content of the molecules. In the absence of H-2M, Ek/b molecules contained a more heterogeneous set of class II-associated invariant chain peptides (CLIP) than Ab did, which, unlike Ab-CLIP complexes, were not SDS-stable. Unlike Ab molecules, both Ek/b and Ak efficiently presented exogenously added peptides to T cells in the absence of H-2M. In addition, epitopes from some proteins, especially those known to be invariant chain independent, were presented by Ak molecules in the mutant animals. To our surprise, expression of Ek/b overcame the positive selection defect observed in H-2M-deficient mice expressing Ab alone. In contrast, Ak expression did not augment positive selection of CD4+ T cells in the mutant animals. Some of these findings in vivo contrast significantly with findings from in vitro studies on murine MHC class II molecules in human DM-deficient cell lines.

摘要

为了更全面地了解H-2M作为抗原呈递辅助分子的作用,我们研究了不同的MHC II类同种型和等位基因在体内发挥功能对H-2M的依赖程度。我们构建了除突变株中已有的Ab分子外,还表达Ek/b或Ak分子的H-2M缺陷动物,并比较了不同MHC II类分子在细胞表面呈递抗原以供T细胞识别的能力,以及对胸腺中CD4+ T细胞阳性选择的贡献。进行了生化分析以评估MHC II类分子的成熟情况,并确定这些分子的肽含量。在没有H-2M的情况下,Ek/b分子所含的II类相关恒定链肽(CLIP)比Ab分子的更为多样,与Ab-CLIP复合物不同,这些CLIP在SDS中不稳定。与Ab分子不同,在没有H-2M的情况下,Ek/b和Ak都能有效地将外源添加的肽呈递给T细胞。此外,突变动物中的Ak分子呈递了一些蛋白质的表位,尤其是那些已知不依赖恒定链的表位。令我们惊讶的是,Ek/b的表达克服了在仅表达Ab的H-2M缺陷小鼠中观察到的阳性选择缺陷。相反,Ak的表达并没有增强突变动物中CD4+ T细胞的阳性选择。体内的一些研究结果与在人DM缺陷细胞系中对小鼠MHC II类分子进行的体外研究结果形成了显著对比。

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