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用FK506治疗可防止大鼠结肠同种异体移植的排斥反应。

Treatment with FK506 prevents rejection of rat colon allografts.

作者信息

Hashimoto T, Zhong R Z, Garcia B M, Black R T, Behme R J, Duff J H, Grant D R

机构信息

Department of Surgery, University of Western Ontario, London, Canada.

出版信息

Transplantation. 1994 Jun 15;57(11):1548-54.

PMID:7516586
Abstract

Colon transplantation has been proposed as a method to improve the function of an intestinal allograft. The present study examined the risk of colon rejection and the effect of FK506 on colon rejection in BN-->LEW rats with orthotopic bowel transplants. The first 4 groups included rats with untreated allografts (group 1), rats with isografts treated with 0.6 mg/kg FK506 (group 2), rats with allografts treated with 0.6 mg/kg FK506 (group 3), and rats with allografts treated with 0.4 mg/kg FK506 (group 4). In each of these groups (10-12 rats), half of the animals received a small bowel graft only (SB), while the other half received a small bowel, ascending colon, and cecum graft (SBC). The animals were followed daily until they died or were killed at 4 weeks. In group 5, an additional 18 untreated rats with SBC allografts were randomly killed on the third, fifth, seventh, and tenth postoperative days to study the sequential histopathologic and immunopathologic changes of colon rejection. There was no difference in survival, body weight, nutritional parameters, or bacterial contamination after SB and SBC transplantation. Intestinal transit was slower after SBC than SB transplantation (P < 0.05). Sequential histopathologic studies revealed that (1) the severity and time course of colon rejection was similar to small intestine rejection, and (2) the features of colon rejection were similar to ulcerative colitis. There was no evidence of graft-versus-host disease after SBC transplantation. In summary, adding a segment of large bowel to a small bowel allograft does not increase the risk of rejection or surgical complications. The transplanted colon slows intestinal transit. Treatment with FK506 effectively prevents colon rejection. These data suggest that adding a colon graft may improve the outcome of clinical small bowel transplantation.

摘要

结肠移植已被提议作为一种改善肠道同种异体移植功能的方法。本研究检测了原位肠道移植的BN→LEW大鼠结肠排斥反应的风险以及FK506对结肠排斥反应的影响。前4组包括未处理同种异体移植的大鼠(第1组)、接受0.6mg/kg FK506处理的同基因移植大鼠(第2组)、接受0.6mg/kg FK506处理的同种异体移植大鼠(第3组)以及接受0.4mg/kg FK506处理的同种异体移植大鼠(第4组)。在这些组中的每组(10 - 12只大鼠),一半动物仅接受小肠移植(SB),而另一半接受小肠、升结肠和盲肠移植(SBC)。每天对动物进行观察,直至其死亡或在4周时被处死。在第5组中,另外18只未处理的SBC同种异体移植大鼠在术后第3、5、7和10天被随机处死,以研究结肠排斥反应的序贯组织病理学和免疫病理学变化。SB和SBC移植后在生存率、体重、营养参数或细菌污染方面无差异。SBC移植后肠道转运比SB移植慢(P < 0.05)。序贯组织病理学研究显示:(1)结肠排斥反应的严重程度和时间进程与小肠排斥反应相似,(2)结肠排斥反应的特征与溃疡性结肠炎相似。SBC移植后无移植物抗宿主病的证据。总之,在小肠同种异体移植中添加一段大肠不会增加排斥反应风险或手术并发症。移植的结肠会减缓肠道转运。FK506治疗可有效预防结肠排斥反应。这些数据表明添加结肠移植物可能改善临床小肠移植的结果。

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