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基于 BRGS 的 HLA-A2/-DR2 转基因人类免疫系统小鼠中加速的胸腺生成和改善的 T 细胞反应。

Accelerated thymopoiesis and improved T-cell responses in HLA-A2/-DR2 transgenic BRGS-based human immune system mice.

机构信息

Inserm U1223, Paris, France.

Innate Immunity Unit, Institut Pasteur, Paris, France.

出版信息

Eur J Immunol. 2019 Jun;49(6):954-965. doi: 10.1002/eji.201848001. Epub 2019 Apr 2.

Abstract

Human immune system (HIS) mouse models provide a robust in vivo platform to study human immunity. Nevertheless, the signals that guide human lymphocyte differentiation in HIS mice remain poorly understood. Here, we have developed a novel Balb/c Rag2 Il2rg Sirpa (BRGS) HIS mouse model expressing human HLA-A2 and -DR2 transgenes (BRGSA2DR2). When comparing BRGS and BRGSA2DR2 HIS mice engrafted with human CD34 stem cells, a more rapid emergence of T cells in the circulation of hosts bearing human HLA was shown, which may reflect a more efficient human T-cell development in the mouse thymus. Development of CD4 and CD8 T cells was accelerated in BRGSA2DR2 HIS mice and generated more balanced B and T-cell compartments in peripheral lymphoid organs. Both B- and T-cell function appeared enhanced in the presence of human HLA transgenes with higher levels of class switched Ig, increased percentages of polyfunctional T cells and clear evidence for antigen-specific T-cell responses following immunization. Taken together, the presence of human HLA class I and II molecules can improve multiple aspects of human B- and T-cell homeostasis and function in the BRGS-based HIS mouse model.

摘要

人类免疫系统(HIS)小鼠模型为研究人类免疫提供了强大的体内研究平台。然而,指导 HIS 小鼠中人类淋巴细胞分化的信号仍知之甚少。在这里,我们开发了一种新型的表达人 HLA-A2 和 -DR2 转基因的 Balb/c Rag2 Il2rg Sirpa(BRGS)HIS 小鼠模型(BRGSA2DR2)。当比较 BRGS 和 BRGSA2DR2 HIS 小鼠移植人 CD34 干细胞时,显示出携带人 HLA 的宿主循环中 T 细胞更快出现,这可能反映出小鼠胸腺中更有效的人类 T 细胞发育。BRGSA2DR2 HIS 小鼠中 CD4 和 CD8 T 细胞的发育加快,并在外周淋巴器官中产生更平衡的 B 和 T 细胞区室。在存在人 HLA 转基因的情况下,B 细胞和 T 细胞的功能似乎都增强了,表现为类别转换 Ig 水平升高、多功能 T 细胞的百分比增加以及免疫接种后抗原特异性 T 细胞反应的明显证据。总之,人 HLA I 类和 II 类分子的存在可以改善基于 BRGS 的 HIS 小鼠模型中人类 B 细胞和 T 细胞的多个方面的稳态和功能。

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