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用于在体内追踪同种异体特异性CD4 T细胞激活和耐受的新型TCR转基因模型。

New TCR transgenic model for tracking allospecific CD4 T-cell activation and tolerance in vivo.

作者信息

Sandner Sigrid E, Salama Alan D, Houser Stuart L, Palmer Ed, Turka Laurence A, Sayegh Mohamed H

机构信息

Division of Nephrology, The Children's Hospital, Harvard Medical School, Boston, MA, USA.

出版信息

Am J Transplant. 2003 Oct;3(10):1242-50. doi: 10.1046/j.1600-6143.2003.00220.x.

Abstract

We have developed an adoptive transfer model system to visualize the dynamics of alloantigen-specific CD4+ T-cell activation in vivo. Using TCR-transgenic (tg) mice reactive to I-Ab(m12), we studied the clonal expansion and differentiation of alloreactive T cells by tracking the fate of adoptively transferred TCR-tg CD4+ T cells in syngeneic mice transplanted with skin grafts expressing I-Ab(m12). Following transplantation, alloantigen-specific TCR-tg CD4+ T-cell expansion was observed initially in the draining lymph nodes followed by the spleen. TCR-tg CD4+ T cells up-regulated CD69 and CD25 expression, developed an effector/memory surface phenotype and produced IFN-gamma in response to alloantigen ex vivo. Furthermore, we validate the model system as a means for studying the effects of tolerogenic regimens on alloreactive CD4+ T cells, demonstrating that CTLA4Ig inhibits alloantigen-dependent clonal expansion and effector function of TCR-tg CD4+ T cells in vivo. We describe the first model for tracking alloreactive CD4+ T-cell activation in vivo. It provides a powerful tool for studying CD4+ T-cell mediated alloimmune responses and mechanisms of tolerance induction in vivo.

摘要

我们开发了一种过继转移模型系统,以可视化体内同种异体抗原特异性CD4+ T细胞激活的动态过程。利用对I-Ab(m12)有反应的TCR转基因(tg)小鼠,我们通过追踪过继转移的TCR-tg CD4+ T细胞在移植了表达I-Ab(m12)皮肤移植物的同基因小鼠中的命运,研究了同种反应性T细胞的克隆扩增和分化。移植后,最初在引流淋巴结中观察到同种异体抗原特异性TCR-tg CD4+ T细胞扩增,随后在脾脏中出现扩增。TCR-tg CD4+ T细胞上调CD69和CD25表达,形成效应/记忆表面表型,并在体外对同种异体抗原产生γ干扰素。此外,我们验证了该模型系统作为研究耐受性方案对同种反应性CD4+ T细胞影响的一种手段,证明CTLA4Ig在体内抑制TCR-tg CD4+ T细胞的同种异体抗原依赖性克隆扩增和效应功能。我们描述了第一个用于追踪体内同种反应性CD4+ T细胞激活的模型。它为研究CD4+ T细胞介导的同种免疫反应和体内耐受性诱导机制提供了一个强大的工具。

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