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HLA的结构与功能:当代观点

HLA structure and function: a contemporary view.

作者信息

Bodmer W F

出版信息

Tissue Antigens. 1981 Jan;17(1):9-20. doi: 10.1111/j.1399-0039.1981.tb00661.x.

Abstract

The HLA and H-2 genetic maps are aligned optimally if HLA-A corresponds to H-2K, in which case the position of all the other markers, except these, corresponds. The two sequences could be related by a double inversion, an intra-chromosomal double crossover, or differential expression of different parts of the regions in the two species. The coding regions of DNA are probably arranged into non-contiguous pieces, which may correspond to defined domains of the HLA protein products. Serological data suggests an ABC common region which codes for a piece common to the HLA-A,B and C products and raises the question of control of expression over relatively long distances. Trophoblasts and so choriocarcinomas do not express HLA-A,B,C on their surface and this may explain why the fetus survives as an allograft and why HLA incompatibility does not affect choriocarcinomas. The lack of expression of HLA-A,B,C on some tumors may be a change that is selected for during tumor progression to escape from T cell mediated immune attack. The mouse H-2 I-A region probably corresponds to the neighborhood of HLA-DR, while the apparent heterogeneity of the HLA-DR products may be explained by the existence of two more two set of products homologous to I-A and I-E/C. HLA-A,B,C and DR products may behave like complement components on the cell surface in relation to the T-cell receptor. This suggestion has interesting implications for the function of the T-cell receptor, the nature of antigen specific factors and their role in autoimmune disease. The HLA region as a whole may code for up to 150 peptides of the approximate size of the HLA-A,B and C products.

摘要

如果HLA - A对应于H - 2K,那么HLA和H - 2基因图谱就能实现最佳比对,在这种情况下,除了这些之外的所有其他标记的位置也都对应。这两个序列可能通过双倒位、染色体内双交换或两个物种中区域不同部分的差异表达而相关。DNA的编码区可能排列成不连续的片段,这可能对应于HLA蛋白产物的特定结构域。血清学数据表明存在一个ABC共同区域,它编码HLA - A、B和C产物共有的一段序列,并引发了关于相对远距离表达调控的问题。滋养层细胞以及绒毛膜癌在其表面不表达HLA - A、B、C,这或许可以解释为什么胎儿作为同种异体移植物能够存活,以及为什么HLA不相容性不会影响绒毛膜癌。某些肿瘤上缺乏HLA - A、B、C的表达可能是在肿瘤进展过程中为逃避T细胞介导的免疫攻击而选择的一种变化。小鼠的H - 2 I - A区域可能对应于HLA - DR的邻近区域,而HLA - DR产物明显的异质性可能是由于存在另外两组与I - A和I - E/C同源的产物。HLA - A、B、C和DR产物在细胞表面相对于T细胞受体的行为可能类似于补体成分。这一推测对于T细胞受体的功能、抗原特异性因子的性质及其在自身免疫性疾病中的作用具有有趣的启示。整个HLA区域可能编码多达150种大小近似于HLA - A、B和C产物的肽段。

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