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通过种间外显子洗牌构建新型I类组织相容性抗原。

Construction of novel class I histocompatibility antigens by interspecies exon shuffling.

作者信息

Engelhard V H, Yannelli J R, Evans G A, Walk S F, Holterman M J

出版信息

J Immunol. 1985 Jun;134(6):4218-25.

PMID:2985705
Abstract

Human and mouse class I histocompatibility antigens share considerable structural homology at both the protein and DNA sequence level. This homology has allowed the production of hybrid class I molecules by the reciprocal exchange of DNA sequences corresponding to equivalent domains of HLA-B7 and either H-2Ld or H-2Dd. It is shown that these genes give rise to protein products that are stably expressed on the surface of murine L cells after DNA-mediated gene transfer. These proteins express only those monoclonal antibody-defined H-2 determinants that are expected based on their genetic construction. The molecules have allowed the localization of a number of polymorphic and monomorphic HLA-specific epitopes. In all but one case, expression of an epitope on a domain does not appear to be influenced by the replacement of adjacent human domains with their murine equivalents, suggesting a considerable degree of structural independence of the domains. Cells expressing the hybrid molecules have also been tested as targets for a panel of HLA-B7-specific cytotoxic T cell clones. The results show that the polymorphic determinants recognized by these clones map to the alpha 1 and alpha 2 domains of the HLA-B7 molecule. No evidence for an influence of species-related amino acid sequence differences in the third extracellular domain on T cell recognition was seen. The results are discussed in light of the proposed domain structure of the class I proteins and the potential use of such molecules for further functional studies.

摘要

人类和小鼠的I类组织相容性抗原在蛋白质和DNA序列水平上都具有相当大的结构同源性。这种同源性使得通过对应于HLA - B7与H - 2Ld或H - 2Dd等效结构域的DNA序列的相互交换来产生杂交I类分子成为可能。结果表明,这些基因在DNA介导的基因转移后产生的蛋白质产物能在小鼠L细胞表面稳定表达。这些蛋白质仅表达那些基于其基因构建预期的单克隆抗体定义的H - 2决定簇。这些分子已使许多多态性和单态性HLA特异性表位得以定位。除一种情况外,在一个结构域上表位的表达似乎不受相邻人类结构域被其小鼠等效结构域替换的影响,这表明各结构域具有相当程度的结构独立性。表达杂交分子的细胞也已被用作一组HLA - B7特异性细胞毒性T细胞克隆的靶细胞进行测试。结果表明,这些克隆识别的多态性决定簇定位于HLA - B7分子的α1和α2结构域。未观察到第三细胞外结构域中物种相关氨基酸序列差异对T细胞识别有影响的证据。根据I类蛋白质的提议结构域结构以及此类分子在进一步功能研究中的潜在用途对结果进行了讨论。

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