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对抹香鲸肌红蛋白免疫反应的遗传控制及不同位点间的影响。

Genetic control and intersite influences on the immune response to sperm whale myoglobin.

作者信息

David C S, Atassi M Z

出版信息

Adv Exp Med Biol. 1982;150:97-125. doi: 10.1007/978-1-4684-4331-8_6.

Abstract

Determination of the precise antigenic structure of sperm-whale myoglobin (Mb) has enabled us to focus our attention on the molecular and cellular factors that control and regulate the immune responses to the protein antigen. Our studies have shown that the immune responses to sperm-whale Mb are controlled by genes in the I region of the major histocompatibility complex (H-2) of mice. More importantly, the responses to the synthetic antigenic sites are each under separate genetic control. The recognition of the antigenic sites by antibodies is independent of the immunized species and of the time the antisera are obtained after the initial immunization (from nine days up to a year). The same sites are recognized by antisera raised in rabbit, goat, pig, cat, chicken and outbred and inbred mice. The same sites recognized by mouse B-cells are also recognized by mouse T-cells. No meaningful genetic control of antibody affinity was observed. Autoimmune antibody and T-lymphocyte proliferative responses were readily generated by immunizing an animal with self-Mb. With mouse Mb, the autoimmune T-lymphocyte response was under genetic control and mapped with the I-A and the H-2D end of the H-2 gene complex. In other recent studies we have shown, using several Mb variants, that the binding capacity of an antigenic site is fully accounted for by substitutions in the antigenic sites (actual contact residues) and in residues close (within 7.A) to the sites (i.e. environmental residues). The overall response to Mb is regulated by inter-site influences which can either be of a cooperative (help) nature or of a suppressive nature. Finally, genetic control of the responses to individual antigenic sites on a protein is not only determined by the genetic constitution of the host but also by the chemical properties of the individual sites. The H-2 subregions mapping the responses to given antigenic sites can also recognize other sites, which were previously unrecognizable in a homologous protein, if the chemical properties of these sites are suitably altered.

摘要

对抹香鲸肌红蛋白(Mb)精确抗原结构的测定,使我们能够将注意力集中在控制和调节针对该蛋白质抗原免疫反应的分子和细胞因素上。我们的研究表明,对抹香鲸Mb的免疫反应受小鼠主要组织相容性复合体(H-2)I区基因的控制。更重要的是,对合成抗原位点的反应各自受独立的遗传控制。抗体对抗原位点的识别与免疫物种以及初次免疫后获得抗血清的时间无关(从九天到一年)。兔、山羊、猪、猫、鸡以及远交和近交小鼠产生的抗血清都能识别相同的位点。小鼠B细胞识别的相同位点也能被小鼠T细胞识别。未观察到抗体亲和力有意义的遗传控制。用自身Mb免疫动物很容易产生自身免疫抗体和T淋巴细胞增殖反应。对于小鼠Mb,自身免疫T淋巴细胞反应受遗传控制,并定位在H-2基因复合体的I-A和H-2D末端。在最近的其他研究中,我们使用几种Mb变体表明,抗原位点的结合能力完全由抗原位点(实际接触残基)以及与该位点接近(在7埃范围内)的残基(即环境残基)中的取代所决定。对Mb的总体反应受位点间影响的调节,这些影响可以是协同(促进)性质的,也可以是抑制性质的。最后,对蛋白质上单个抗原位点反应的遗传控制不仅取决于宿主的遗传构成,还取决于各个位点的化学性质。如果这些位点的化学性质适当改变,定位对给定抗原位点反应的H-2亚区也能识别同源蛋白质中以前无法识别的其他位点。

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