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FTY720减少T细胞向小鼠肠道移植组织的募集,并防止移植组织浸润细胞的激活。

FTY720 reduces T-cell recruitment into murine intestinal allograft and prevents activation of graft-infiltrating cells.

作者信息

Kimura Takuya, Hasegawa Toshimichi, Nakai Hiroshi, Azuma Tatsuo, Usui Noriaki, Sasaki Takashi, Okada Akira

机构信息

Department of Pediatric Surgery, Osaka University Graduate School of Medicine, Japan.

出版信息

Transplantation. 2003 May 15;75(9):1469-74. doi: 10.1097/01.TP.0000058816.13525.92.

Abstract

BACKGROUND

Effective immunosuppression is a critical determinant of graft survival in small-bowel transplantation (SBTx). The present study was designed to determine the potency of FTY720, a newly synthesized immunosuppressant, in rat SBTx and examine the phenotype of graft-infiltrating cells to evaluate its effect on intestinal allografts.

MATERIALS AND METHODS

A segment of intestine of Dark Agouti rats was transplanted heterotopically into Lewis rats. The recipients were treated with or without oral FTY720 at a dose of 1 mg/kg per day. Six days after surgery, peripheral blood lymphocytes and lymphocytes from the mesenteric lymph nodes, Peyer's patches, intraepithelial site, and lamina propria of the intestinal allograft were isolated. After the number of lymphocytes in each site was counted, the lymphocyte subpopulations in the intestinal allograft were evaluated by means of a FACScan flow cytometer using several monoclonal antibodies.

RESULTS

FTY720 treatment significantly prolonged recipient survival and strongly inhibited rejection histologically in comparison with control rats. FTY720 immunosuppression resulted in a marked reduction of lymphocyte number in the graft epithelium and lamina propria and the proportion of CD8+ and CD25+ cells. FTY720 also significantly decreased T-cell receptors and increased B cells in the graft Peyer's patches.

CONCLUSION

FTY720 promoted long-term SBTx recipient survival and maintained the architecture of intestinal allografts. FTY720 immunosuppression may be associated with a reduction of T-cell recruitment subsequent to the redistribution of lymphocyte subpopulations to control the proliferation and activation of graft-infiltrating cells in intestinal allografts.

摘要

背景

有效的免疫抑制是小肠移植(SBTx)中移植物存活的关键决定因素。本研究旨在确定新合成的免疫抑制剂FTY720在大鼠SBTx中的效力,并检查移植物浸润细胞的表型,以评估其对小肠同种异体移植物的影响。

材料与方法

将一段深色刺豚鼠的小肠异位移植到Lewis大鼠体内。接受者接受或不接受每天1mg/kg剂量的口服FTY720治疗。术后6天,分离外周血淋巴细胞以及来自肠系膜淋巴结、派尔集合淋巴结、肠同种异体移植物上皮内部位和固有层的淋巴细胞。在对每个部位的淋巴细胞数量进行计数后,使用几种单克隆抗体通过FACScan流式细胞仪评估肠同种异体移植物中的淋巴细胞亚群。

结果

与对照大鼠相比,FTY720治疗显著延长了接受者的存活时间,并在组织学上强烈抑制了排斥反应。FTY720免疫抑制导致移植物上皮和固有层中淋巴细胞数量以及CD8+和CD25+细胞比例显著降低。FTY720还显著减少了移植物派尔集合淋巴结中的T细胞受体并增加了B细胞。

结论

FTY720促进了SBTx接受者的长期存活并维持了小肠同种异体移植物的结构。FTY720免疫抑制可能与淋巴细胞亚群重新分布后T细胞募集减少有关,从而控制小肠同种异体移植物中移植物浸润细胞的增殖和活化。

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