Binz H, Wigzell H
J Exp Med. 1975 Jul 1;142(1):197-211. doi: 10.1084/jem.142.1.197.
Antigen-binding receptors on T lymphocytes and IgG antibodies with the same antigen-binding specificity as the T-cell receptors display shared or identical idiotypes. This was shown using a system where adult F1 hybrid rats between two inbred strains were inoculated with T lymphocytes from one parental strain. Such F1 hybrid rats produce antibodies directed against idiotypic determinants present on IgG alloantibodies, produced in the T donor genotype strain and with specificity for the alloantigens of the other parental strain. The idiotypic nature of the F1 antialloantibody serum against the parental alloantibodies was demonstrated both by indirect hemagglutination tests or by gel diffusion using alloantisera with different specificity as targets. Furthermore, the F1 anti-T-lymphocyte sera could be shown to contain antibodies against idiotypic parental T lymphocytes as well. This was shown by the capacity of the antisera, in the presence of complement, to wipe out the relevant parental T-cell reactivity against the other parental strain (as measured in MLC or GVH) whilst leaving the T-lymphocyte reactivity against a third, unrelated allogeneic strain intact. These findings demonstrate that F1 hybrid rats inoculated with parental T lymphocytes make anti-idiotypic antibodies directed against both the T cell receptors and IgG alloantibodies of that parental strain with specificity for alloantigens of the other parental strain. In order to prove identity between the anti-idiotypic antibodies against the B and T-cell antigen-binding molecules the following experiments were carried out; highly purified IgG from relevant alloantibody-containing serum in immunosorbent from could be shown to selectively remove both anti-idiotypic activities from the F1 antiserum. Further more, parental normal T lymphocytes could be shown capable of removing from the anti-idiotypic antisera all those antibodies that would cause agglutination of the relevant alloantibody-coated erythrocytes in the indirect agglutination assay. We would thus conclude that T and B lymphocytes reactive against a given antigenic determinant use receptors with antigen-binding areas coded for by the same variable gene subset(s).
T淋巴细胞上的抗原结合受体以及与T细胞受体具有相同抗原结合特异性的IgG抗体,表现出共同或相同的独特型。这是通过一个系统得以证明的,在该系统中,将两个近交系之间的成年F1杂种大鼠用来自一个亲本品系的T淋巴细胞进行接种。此类F1杂种大鼠产生针对存在于IgG同种抗体上独特型决定簇的抗体,这些同种抗体由T供体基因型品系产生,且对另一亲本品系的同种抗原有特异性。通过间接血凝试验或使用具有不同特异性的同种抗血清作为靶标的凝胶扩散试验,均证实了F1抗同种抗体血清针对亲本品系同种抗体的独特型性质。此外,F1抗T淋巴细胞血清也可被证明含有针对亲本品系独特型T淋巴细胞的抗体。这是通过抗血清在补体存在的情况下能够消除相关亲本品系T细胞针对另一亲本品系的反应性(如在混合淋巴细胞培养或移植物抗宿主反应中所测定)得以显示的,而同时使T淋巴细胞针对第三个无关同种异体品系的反应性保持完整。这些发现表明,接种亲本品系T淋巴细胞的F1杂种大鼠产生针对该亲本品系T细胞受体和IgG同种抗体的抗独特型抗体,这些抗体对另一亲本品系的同种抗原有特异性。为了证明针对B细胞和T细胞抗原结合分子的抗独特型抗体之间的同一性,进行了以下实验;来自免疫吸附中相关含同种抗体血清的高度纯化IgG可被证明能从F1抗血清中选择性地去除两种抗独特型活性。此外,亲本品系正常T淋巴细胞能够从抗独特型抗血清中去除所有那些在间接凝集试验中会导致相关同种抗体包被红细胞凝集的抗体。因此我们可以得出结论,针对给定抗原决定簇产生反应的T淋巴细胞和B淋巴细胞使用由相同可变基因亚群编码抗原结合区的受体。