首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Redistribution of renal allograft-responding leukocytes during rejection. II. Kinetics and specificity
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Redistribution of renal allograft-responding leukocytes during rejection. II. Kinetics and specificity

机译:排斥过程中肾脏同种异体移植反应白细胞的重新分布。二。动力学和特异性

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摘要

We investigated the traffic of allograft-responding leukocytes between the host and graft without handling of these cells in vitro. The blood flow between the host and graft was disconnected, the proliferating cells were labeled with [3H]thymidine selectively in the graft or in the host, the label was chased with cold thymidine, and the circulation was reestablished. The localization of labeled cells was quantitated by autoradiography. The first host-derived labeled cells appeared in the graft and graft-derived labeled cells in the host, already on the 1st d after transplantation. This was followed by an exponential increase in the labeled cell traffic in both directions. The peak of traffic was observed on day 4 after transplantation, whereafter the traffic rapidly declined and tapered off. This decline was not due to exhaustion of supply, as the labeled cells continued to proliferate in their original compartments, nor to a slowdown of blood circulation, which took place 2-3 d later. We consider the decline to indicate that the rejection has proceeded to a (irreversible) stage autonomous of the host lymphatic and hematopoietic system. During the exponential increase, nearly one- third of the graft-infiltrating inflammatory cells were replaced as a consequence of relocalization during each 18-h-period. All mononuclear white cell types, with the exception of granulocytes, participated in the traffic. Most lymphoid cells entrapped in the graft were descendents of recent cell divisions; most of the mononuclear phagocytes derived from a preexisting phagocyte pool. The entrapment of labeled leukocytes in a relevant graft was specific: when an allograft and an autograft were simultaneously transplanted, a more than 50-fold entrapment was observed in the allograft, compared with the autograft. Very few of the cells localized in irrelevant positions, such as the liver and lung, of the recipient.
机译:我们调查了宿主和移植物之间同种异体移植反应白细胞的流量,而没有在体外处理这些细胞。断开宿主与移植物之间的血流,在移植物中或在宿主中用[3H]胸苷选择性标记增殖细胞,用冷胸苷追踪标记物,并重新建立循环。通过放射自显影定量标记细胞的定位。第一个宿主来源的标记细胞出现在移植物中,而宿主中的移植物来源标记的细胞出现在移植后的第一天。随后,在两个方向上标记的小区流量都呈指数增长。移植后第4天观察到交通高峰,此后交通迅速下降并逐渐减少。这种下降不是由于供应不足,因为标记的细胞继续在其原始隔室中增殖,也不是由于血液循环减慢,后者在2-3天后发生。我们认为这种下降表明排斥反应已经进行到宿主淋巴和造血系统自主的(不可逆)阶段。在指数增加期间,由于在每个18小时的周期内重新定位,将近三分之一的移植物浸润性炎症细胞被替换。除粒细胞外,所有单核白细胞类型都参与了运输。移植物中截留的大多数淋巴样细胞是最近细胞分裂的后代。大多数单核吞噬细胞均来自先前存在的吞噬细胞池。标记的白细胞在相关移植物中的包埋是特定的:当同种异体移植物和自体移植物同时移植时,与同种异体移植物相比,观察到同种异体移植物中有超过50倍的包被。很少有细胞位于受体的无关位置,如肝和肺。

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