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具有明确的I类抗原免疫反应基因的同基因大鼠品系中的移植排斥反应。II. 全单倍型错配中Ir基因功能的定量方面。

Graft rejection in a congenic panel of rats with defined immune response genes for class I antigens. II. Quantitative aspects of Ir gene function in a full-haplotype mismatch.

作者信息

Stewart R, Stephenson P, Godden U, Butcher G, Roser B

出版信息

Transplantation. 1985 Oct;40(4):432-6. doi: 10.1097/00007890-198510000-00017.

Abstract

Previous studies have shown that the Ir-gene-controlled rejection of rl tissues by c/u responder and non-rejection by c low responders does not extend to tissues expressing a full a haplotype mismatch. However, antibody responses and liver graft rejection are both defective in low responders, even across a full haplotype barrier. We have therefore used a titrated adoptive transfer assay to search for quantitative differences in the responsiveness of c and c/u animals to a organ grafts. We first established that a heart graft rejection could be ablated in both recipient strains with whole-body irradiation and could be restored with syngeneic cells. Titration of restorative cells revealed that 5 times as many c cells were required to restore graft rejection in c recipients as c/u cells were required in c/u recipients. Use of cells from primed donors showed that in both c/u and c animals these cells had undergone about a 5-fold increase in potency, showing that there was no failure of proliferation and differentiation in the low responder after contact with antigens. Cross-transfer experiments were done to attempt to localize the defect in low-responder animals either to a failure of low-responder antigen-presenting cells (APC) to trigger a response or a defect in the responsiveness of alloreactive cells toward the a antigens. In these experiments c cells were obtained from radiation chimeras of the c----c/u type. These cells were used to restore graft rejection in c/u irradiated recipients. Similar experiments employing c/u cells obtained from c/u----c chimeras and given to irradiated c recipients were also done. These showed that c cells from chimeras were marginally less potent than c/u cells from chimeras. In contrast when cross-transfer of c/u cells to c animals bearing a nonrejected rl heart was done, no rejection was seen even when antigen presenting cells were cotransferred. The conclusions from this series of experiments were that quantitatively small defects were present in both repertoire and antigen presentation, and that these quantitative defects in aggregate were probably sufficient to explain the documented low responsiveness of c animals to the a haplotype. The failure of high-responder c/u cells to secure rejection of rl tissues in the low-responder c environment suggests that presentation of isolated class I differences in host APCs is mandatory for rejection to occur and is highly defective in the c animal.

摘要

先前的研究表明,Ir基因控制的c/u反应者对rl组织的排斥以及c低反应者对其的不排斥现象,并不适用于表达完全a单倍型错配的组织。然而,低反应者的抗体反应和肝移植排斥反应均存在缺陷,即使跨越完全单倍型屏障也是如此。因此,我们采用了滴定过继转移试验,以寻找c和c/u动物对a器官移植反应性的定量差异。我们首先确定,通过全身照射可消除两种受体品系的心脏移植排斥反应,并可通过同基因细胞恢复。对恢复性细胞的滴定显示,在c受体中恢复移植排斥反应所需的c细胞数量是c/u受体中所需c/u细胞数量的5倍。使用致敏供体的细胞表明,在c/u和c动物中,这些细胞的效力均增加了约5倍,这表明低反应者在接触抗原后,其增殖和分化并未出现障碍。进行了交叉转移实验,试图将低反应者动物的缺陷定位为低反应者抗原呈递细胞(APC)触发反应失败,或同种反应性细胞对a抗原反应性的缺陷。在这些实验中,c细胞取自c----c/u型辐射嵌合体。这些细胞用于恢复经照射的c/u受体的移植排斥反应。还进行了类似的实验,采用从c/u----c嵌合体获得的c/u细胞,并将其给予经照射的c受体。这些结果表明,嵌合体来源的c细胞的效力略低于嵌合体来源的c/u细胞。相反,当将c/u细胞交叉转移至携带未被排斥的rl心脏的c动物时,即使同时转移抗原呈递细胞,也未观察到排斥反应。这一系列实验的结论是,在库和抗原呈递方面均存在数量上较小的缺陷,并且这些累积的定量缺陷可能足以解释所记录的c动物对a单倍型的低反应性。高反应性的c/u细胞在低反应性的c环境中无法确保对rl组织的排斥,这表明宿主APC中单独的I类差异的呈递是排斥反应发生所必需的,并且在c动物中存在高度缺陷。

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