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将α3结构域引入HLA B27后转基因小鼠中出现强烈的异种HLA反应。

Strong xenogeneic HLA response in transgenic mice after introducing an alpha 3 domain into HLA B27.

作者信息

Kalinke U, Arnold B, Hämmerling G J

机构信息

German Cancer Research Center, Institute of Immunology and Genetics, Heidelberg.

出版信息

Nature. 1990 Dec 13;348(6302):642-4. doi: 10.1038/348642a0.

Abstract

The pronounced response by mouse T cells to the major histocompatibility complex (MHC) class I antigens of the same species is characterized by a relatively large fraction of responding cells. Responses to MHC class I allelles of other species are, however, generally much weaker. T lymphocytes are positively selected on thymic MHC antigens, resulting in a T-cell repertoire with strong alloreactivity. This has been explained in terms of a mouse T-cell repertoire that is not efficiently selected for recognition of HLA molecules owing to the absence of HLA in mice. Here we show that mice transgenic for HLA mount a T-cell response against allogeneic HLA that is no better than in normal mice. We decided instead to test whether the mouse accessory molecule Lyt-2 on cytotoxic T lymphocytes could interact efficiently with the alpha 3 domain of HLA. To do this, we replaced the alpha 3 domain of HLA-B27 by a murine alpha 3 domain in a gene construct used to produce transgenic mice, and then used the spleen cells from these mice to stimulate normal mouse T cells. Under these conditions cytotoxic T lymphocytes were generated with the same frequency against xenogeneic HLA-B27 determinants as against allogeneic mouse class I antigens. These findings indicate that the normally weak xeno-MHC response is due to the inefficient interaction of the murine Lyt-2 accessory molecule with HLA class I, and not to limitations of the mouse T-cell repertoire.

摘要

小鼠T细胞对同一物种主要组织相容性复合体(MHC)I类抗原的显著反应,其特征在于有相对较大比例的反应细胞。然而,对其他物种MHC I类等位基因的反应通常要弱得多。T淋巴细胞在胸腺MHC抗原上进行阳性选择,从而产生具有强烈同种异体反应性的T细胞库。这一点已根据小鼠T细胞库来解释,即由于小鼠中不存在HLA,所以没有有效地选择该T细胞库来识别HLA分子。在此我们表明,转染了HLA的小鼠针对同种异体HLA产生的T细胞反应并不比正常小鼠更好。相反,我们决定测试细胞毒性T淋巴细胞上的小鼠辅助分子Lyt-2是否能与HLA的α3结构域有效相互作用。为此,我们在用于产生转基因小鼠的基因构建体中,用鼠α3结构域替换了HLA-B27的α3结构域,然后用这些小鼠的脾细胞刺激正常小鼠T细胞。在这些条件下,产生细胞毒性T淋巴细胞针对异种HLA-B27决定簇的频率与针对同种异体小鼠I类抗原的频率相同。这些发现表明,正常情况下较弱的异种MHC反应是由于鼠Lyt-2辅助分子与HLA I类的相互作用效率低下,而不是由于小鼠T细胞库的限制。

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