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T细胞受体:种系多态性及在脱髓鞘疾病中的使用模式

T-cell receptors: germline polymorphism and patterns of usage in demyelinating diseases.

作者信息

Usuku K, Joshi N, Hauser S L

机构信息

UCSF School of Medicine, Department of Neurology 94143-0114.

出版信息

Crit Rev Immunol. 1992;11(6):381-93.

PMID:1382445
Abstract

The genomic organization of the T-cell receptor (TCR) gene complexes accounts for many central aspects of T-cell immunobiology, including specificity and diversity. Recent data indicate that polymorphism of TCR genes is present within a species and may influence the immune phenotype of an individual. Such polymorphism has been detected by RFLP, by the presence of large regions of insertion or deletion of germline DNA, and by allelic variability of individual gene segments that are expressed. In addition to allelic variation of TCR genes, immune responses may also be influenced by the repertoire of the TCR molecules that are expressed by responding T-cell populations. In some situations, pathogenic T-cell responses may involve expression of limited numbers of TCR gene families. This is true, for example, in experimental allergic encephalomyelitis, an autoimmune nervous system disease mediated by T-cells reactive to myelin basic protein. In the human disease counterpart, multiple sclerosis, a more complex pattern of T-cell recognition to the putative autoantigen is generally present, although in some individuals a restricted response may occur. Specific therapies targeted to certain TCR molecules represents a promising approach to chronic inflammatory diseases in humans. The efficacy of such therapies will be determined in part by the TCR repertoire expressed in individual disease situations and by the potential for plasticity in the pathogenic T-cell response that may exist.

摘要

T细胞受体(TCR)基因复合体的基因组组织解释了T细胞免疫生物学的许多核心方面,包括特异性和多样性。最近的数据表明,TCR基因的多态性存在于一个物种内,并且可能影响个体的免疫表型。这种多态性已通过限制性片段长度多态性(RFLP)、种系DNA大片段插入或缺失的存在以及所表达的单个基因片段的等位基因变异性检测到。除了TCR基因的等位基因变异外,免疫反应也可能受到反应性T细胞群体所表达的TCR分子库的影响。在某些情况下,致病性T细胞反应可能涉及有限数量的TCR基因家族的表达。例如,在实验性变应性脑脊髓炎中就是如此,这是一种由对髓鞘碱性蛋白有反应的T细胞介导的自身免疫性神经系统疾病。在人类疾病对应物多发性硬化症中,尽管在某些个体中可能会出现受限反应,但通常存在对假定自身抗原更复杂的T细胞识别模式。针对某些TCR分子的特异性疗法是治疗人类慢性炎症性疾病的一种有前景的方法。此类疗法的疗效将部分取决于个体疾病情况下所表达的TCR库以及致病性T细胞反应中可能存在的可塑性。

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