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识别膜结合抗原的自身反应性B淋巴细胞从外周淋巴组织中清除。

Elimination from peripheral lymphoid tissues of self-reactive B lymphocytes recognizing membrane-bound antigens.

作者信息

Hartley S B, Crosbie J, Brink R, Kantor A B, Basten A, Goodnow C C

机构信息

Centenary Institute of Cancer Medicine and Cell Biology, University of Sydney, New South Wales, Australia.

出版信息

Nature. 1991 Oct 24;353(6346):765-9. doi: 10.1038/353765a0.

Abstract

The long-standing hypothesis that tolerance to self antigens is mediated by either elimination or functional inactivation (anergy) or self-reactive lymphocytes is now accepted, but little is known about the factors responsible for initiating one process rather than the other. In the B-cell lineage, tolerant self-reactive cells persist in the peripheral lymphoid organs of transgenic mice expressing lysozyme and anti-lysozyme immunoglobulin genes, but are eliminated in similar transgenic mice expressing anti-major histocompatibility complex immunoglobulin genes. By modifying the structure of the lysozyme transgene and the isotype of the anti-lysozyme immunoglobulin genes, we demonstrate here that induction of anergy or deletion is not due to differences in antibody affinity or isotype, but to recognition of monomeric or oligomeric soluble antigen versus highly multivalent membrane-bound antigen. Our findings indicate that the degree of receptor crosslinking can have qualitatively distinct signalling consequences for lymphocyte development.

摘要

长期以来的假说认为,对自身抗原的耐受性是由自身反应性淋巴细胞的消除或功能失活(无反应性)介导的,这一假说如今已被接受,但对于启动这一过程而非另一过程的因素却知之甚少。在B细胞谱系中,表达溶菌酶和抗溶菌酶免疫球蛋白基因的转基因小鼠外周淋巴器官中存在耐受的自身反应性细胞,但在表达抗主要组织相容性复合体免疫球蛋白基因的类似转基因小鼠中,这些细胞被消除。通过改变溶菌酶转基因的结构和抗溶菌酶免疫球蛋白基因的同种型,我们在此证明,无反应性或缺失的诱导并非由于抗体亲和力或同种型的差异,而是由于对单体或寡聚可溶性抗原与高度多价膜结合抗原的识别。我们的研究结果表明,受体交联程度对淋巴细胞发育可产生质上不同的信号后果。

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