生物
否定选择
BETA(编程语言)
转基因小鼠
积极选择
分子
小鼠品系
人类白细胞抗原
选择(遗传算法)
抗原
基因
遗传学
分子生物学
转基因
免疫学
化学
基因组
人工智能
程序设计语言
有机化学
计算机科学
作者
Gudrun Strau\,D. A. A. Vignali,G�nther Sch�nrich,G�nterJ. H�mmerling
出处
期刊:Immunogenetics
[Springer Science+Business Media]
日期:1994-06-01
卷期号:40 (2): 104-8
被引量:71
摘要
The establishment of HLA transgenic mice as models for autoimmune disorders requires that the HLA molecules can be efficiently recognized and mediate positive and negative selection of mouse T cells. This question was investigated in DR3(DRw17) transgenic mice back-crossed to the B10.Q(H-2q) strain which does not form mixed mouse-human class II heterodimers. Here we report that efficient negative 5election on DR3(DRw17) molecules was observed for vβ5, 11, and 13 subpopulations of CD4+T cells, but not for vβ4, 7, 8, 9, and 10. vβ5 and 11 cells are also negatively selected by mouse class II E molecules which is the structural homologue to DR molecules. Positive selection on DR3(DRw17) was only observed for vβ6 cells but this was less efficient than positive selection of vβ6 cells by E molecules. The data indicate that DR3(DRw17) molecules select similar subgroups of mouse T cells as E molecules although with slightly different efficiency.
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