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人T细胞在HLA-DR1转基因NOD/scid小鼠胸腺内/脾脏中的植入。

Intra-thymic/splenic engraftment of human T cells in HLA-DR1 transgenic NOD/scid mice.

作者信息

Camacho Ramon E, Wnek Richard, Shah Kashmira, Zaller Dennis M, O'Reilly Richard J, Collins Nancy, Fitzgerald-Bocarsly Patricia, Koo Gloria C

机构信息

Merck Research Laboratories, Rahway, NJ, USA.

出版信息

Cell Immunol. 2004 Nov-Dec;232(1-2):86-95. doi: 10.1016/j.cellimm.2005.02.003. Epub 2005 Apr 19.

Abstract

A HLA-DR1 transgenic mouse (NOD/scid-DR1) was derived by breeding the existing B10.M/J-[Tg]DR1 mouse with the NOD/scid mouse. The intention was to enhance engraftment of human T cells by providing human class II elements in the tissues. Thymus and spleen fragments from adult NOD/scid-DR1 mice were transplanted under the syngeneic kidney capsules, followed by injection of human cord blood mononuclear cells (CBMNC) into transplanted tissues. FACS analyses showed that human T and B cells were consistently detected in the peripheral blood and spleen, of the chimeric mice. An average of 20% of human cells was found in the spleen and the engrafted thymus/spleen tissues. Furthermore, human cells from these tissues could proliferate with anti-human CD3 antibody and these mice could generate humoral and cellular responses to allogeneic human cells. Cytokines, such as IL-10, GMCSF, IFN-gamma, and TNF-alpha were also detected in the supernatants of the cultured human cells from the chimeric mice, when they were stimulated with allogeneic cells. Therefore, a novel mouse model with functional circulating human T and B cells was established that would facilitate the exploration of vaccine, the disease processes of autoimmunity, HIV infection, and human cancer.

摘要

通过将现有的B10.M/J-[Tg]DR1小鼠与NOD/scid小鼠杂交,培育出了一种HLA-DR1转基因小鼠(NOD/scid-DR1)。目的是通过在组织中提供人类II类分子来增强人类T细胞的植入。将成年NOD/scid-DR1小鼠的胸腺和脾脏片段移植到同基因肾被膜下,然后将人类脐血单个核细胞(CBMNC)注射到移植组织中。流式细胞术分析表明,在嵌合小鼠的外周血和脾脏中持续检测到人类T细胞和B细胞。在脾脏以及植入的胸腺/脾脏组织中平均发现20%的人类细胞。此外,来自这些组织的人类细胞能够用抗人CD3抗体增殖,并且这些小鼠能够对异基因人类细胞产生体液和细胞反应。当用异基因细胞刺激时,在来自嵌合小鼠的培养人类细胞的上清液中也检测到了细胞因子,如IL-10、GMCSF、IFN-γ和TNF-α。因此,建立了一种具有功能性循环人类T细胞和B细胞的新型小鼠模型,这将有助于探索疫苗、自身免疫性疾病进程、HIV感染和人类癌症。

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