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The concurrent maturation of mouse and human thymocytes in human fetal thymus implanted in NIH-beige-nude-xid mice is associated with the reconstitution of the murine immune system

机译:NIH-米色裸鼠植入人胎胸腺中小鼠和人胸腺细胞的同时成熟与鼠免疫系统的重建有关

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摘要

To determine whether the human thymus provides an environment for the maturation of murine T cells, human fetal thymus and liver (hu-thy/liv) were implanted into congenitally athymic NIH-beige-nude-xid (BNX) mice or C.B-17 scid/scid (SCID) mice. 3 mo after implantation, in contrast to the hu-thy/liv implant in SCID mice, which was populated only with human CD4/CD8 single- and double-positive thymocytes, the hu-thy/liv implant in BNX mice contained a chimeric population of human and mouse CD4/CD8 single- and double-positive thymocytes. Immunohistochemical staining of the hu-thy/liv implant in BNX mice indicated that the population of double-positive mouse thymocytes was localized to discrete areas of the human fetal thymus. Quantitative improvements in mouse T cell and immunoglobulin (Ig) G parameters were observed after grafting of the human fetal thymus and liver tissue into BNX mice. In addition, in contrast to the nonimplanted BNX mice, the implanted BNX mice were capable of mounting a keyhole limpet hemocyanin-specific IgG response and their peripheral T cells were responsive to stimulation with mitogens and antibodies directed to the T cell receptor. Furthermore, after in vivo priming, T cells present in lymph nodes of the implanted BNX mice were capable of mounting an antigen-induced in vitro T cell-dependent proliferative response. Thus, concurrent with the continued maturation of human T cells, murine T cells differentiated within the human fetal thymus implanted in the BNX mice and mediated the phenotypic and functional reconstitution of the murine immune system. Mice with a reconstituted immune system that contain a human thymic implant that is infectible with human immunodeficiency virus (HIV) should prove useful in the investigation of T cell maturation in the thymus and in the evaluation of potential HIV vaccines.
机译:为了确定人类胸腺是否为鼠T细胞的成熟提供了环境,将人类胎儿胸腺和肝脏(hu-thy / liv)植入了先天性无胸腺NIH-beige-nude-xid(BNX)小鼠或CB-17 scid中/ scid(SCID)小鼠。植入后3个月,与SCID小鼠中的hu-thy / liv植入物仅由人CD4 / CD8单和双阳性胸腺细胞组成的B相反,BNX小鼠中的hu-thy / liv植入物包含嵌合群体人和小鼠CD4 / CD8单和双阳性胸腺细胞的数量。 BNX小鼠中hu-thy / liv植入物的免疫组织化学染色表明,双阳性小鼠胸腺细胞群体位于人胎胸腺的离散区域。将人类胎儿胸腺和肝组织移植到BNX小鼠后,观察到小鼠T细胞和免疫球蛋白(Ig)G参数的定量改善。此外,与未植入的BNX小鼠相反,植入的BNX小鼠能够进行匙孔血蓝蛋白特异性IgG应答,并且其外周T细胞对促细胞分裂剂和针对T细胞受体的抗体的刺激应答。此外,在体内启动后,存在于植入的BNX小鼠的淋巴结中的T细胞能够发起抗原诱导的体外T细胞依赖性增殖反应。因此,与人类T细胞的持续成熟同时,在植入BNX小鼠的人类胎儿胸腺内分化的鼠T细胞介导了鼠免疫系统的表型和功能重建。具有重组的免疫系统的小鼠中含有可感染人类免疫缺陷病毒(HIV)的人类胸腺植入物,应该被证明对研究胸腺T细胞成熟和评估潜在的HIV疫苗有用。

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