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同种异体靶标对间接CD4免疫的不同易感性产生了分裂耐受性。

Differential susceptibility of allogeneic targets to indirect CD4 immunity generates split tolerance.

作者信息

Chan William F N, Razavy Haide, Anderson Colin C

机构信息

Department of Medical Microbiology, Surgical-Medical Research Institute, University of Alberta, Edmonton, Alberta, Canada.

出版信息

J Immunol. 2008 Oct 1;181(7):4603-12. doi: 10.4049/jimmunol.181.7.4603.

Abstract

CD4 T cells frequently help to activate CD8 T and B cells that effect transplant rejection. However, CD4 T cells alone can reject transplants, either directly or indirectly. The relative effectiveness of indirect CD4 immunity in rejecting different types of allogeneic grafts is unknown. To address this, we used a TCR transgenic mouse model in which indirect CD4 alloimmunity alone can be studied. We challenged transgenic recipients with hematopoietic cells and shortly thereafter skin transplants that could only be rejected indirectly, and observed Ag-specific indirect donor B cell and skin rejection, but not T cell elimination, reflecting a state of split tolerance. Deficiency of indirect CD4 alloimmunity in donor T cell rejection was also apparent when acute indirect rejection of donor islets occurred despite generation and maintenance of mixed T cell chimerism, due to migration of the few passenger T cells into recipient circulation. Although passenger lymphocytes delayed indirect islet rejection, they enhanced rejection by a full repertoire capable of both direct and indirect reactivity. Interestingly, the persistence of chimerism was associated with the eventual development of tolerance, as demonstrated by acceptance of donor skin grafts given late to hematopoietic cell recipients, and hyporesponsiveness of transgenic T cells from islet recipients in vitro. Mechanistically, tolerance was recessive and associated with progressive down-regulation of CD4. Collectively, our data indicate that indirect CD4 immunity is not equally destructive toward different types of allogeneic grafts, the deficiency of which generates split tolerance. The futility of these responses can convert immunity into tolerance.

摘要

CD4 T细胞常常有助于激活那些引发移植排斥反应的CD8 T细胞和B细胞。然而,单独的CD4 T细胞也能够直接或间接地排斥移植器官。间接CD4免疫在排斥不同类型的同种异体移植物中的相对效力尚不清楚。为了解决这个问题,我们使用了一种TCR转基因小鼠模型,在该模型中可以单独研究间接CD4同种免疫。我们用造血细胞对转基因受体进行攻击,此后不久又进行只能被间接排斥的皮肤移植,观察到抗原特异性间接供体B细胞和皮肤排斥反应,但没有T细胞清除现象,这反映了一种分裂耐受状态。当尽管产生并维持了混合T细胞嵌合体,但仍发生供体胰岛的急性间接排斥反应时,间接CD4同种免疫在供体T细胞排斥反应中的缺陷也很明显,这是由于少数过客T细胞迁移到受体循环中所致。尽管过客淋巴细胞延迟了间接胰岛排斥反应,但它们通过具有直接和间接反应能力的完整免疫细胞库增强了排斥反应。有趣的是,嵌合体的持续存在与最终的耐受发展有关,这表现为造血细胞受体后期接受供体皮肤移植,以及胰岛受体的转基因T细胞在体外反应低下。从机制上讲,耐受是隐性的,并且与CD4的逐渐下调有关。总体而言,我们的数据表明,间接CD4免疫对不同类型的同种异体移植物的破坏作用并不相同,其缺陷会产生分裂耐受。这些反应的无效性可将免疫转化为耐受。

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