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心脏异种移植中供体细胞的胎儿接种。

Fetal inoculation with donor cells in cardiac xenotransplantation.

作者信息

Shen Z, Mohiuddin M, DiSesa V J

机构信息

Department of Cardiothoracic Surgery, Medical College of Pennsylvania, Philadelphia, USA.

出版信息

Ann Thorac Surg. 1996 Nov;62(5):1360-3. doi: 10.1016/0003-4975(96)00481-X.

Abstract

BACKGROUND

In utero fetal inoculation with allogeneic cells has produced subsequent tolerance to experimental cardiac allografts. We attempted to extend this observation to a model of xenogeneic cardiac transplantation.

METHODS

Lewis rat fetuses were inoculated with Golden Syrian hamster thymocytes (n = 5) or whole spleen cells (n = 5) on the tenth day of intrauterine life. Six weeks after the birth of pretreated fetuses, heterotopic cardiac transplantation using a hamster donor was performed. Three to 4 weeks after parturition, we performed heterotopic cardiac transplantation using hamster donors in the female Lewis rats whose fetuses had been treated in utero.

RESULTS

Animals treated in utero with either thymocytes or whole spleen cells had graft survival of 3 days, not different from that in untreated Lewis rats (n = 5) (p = not significant). Maternal Lewis rats whose fetuses were treated with thymocytes (n = 5) or whole spleen cells (in = 4) had markedly reduced survival of xenogeneic cardiac grafts (range, 3 to 20 hours; mean, 15 hours; p < 0.01; and range, 5 to 15 minutes; mean, 10 minutes; p < 0.01, respectively). Female Lewis rats without intrauterine inoculation (n = 5) had expected xenograft survival time (3 days) (p = not significant). Immunohistochemical staining of hyperacutely rejected grafts showed deposits of immunoglobulin M as well as immunoglobulin G and complement. In normally rejected xenografts, no immunoglobulin M was detected.

CONCLUSIONS

These studies reveal the surprising observation that fetal exposure to xenogeneic cells sensitizes the maternal rat without tolerizing the fetal rat as observed in an allograft model. In addition, whole spleen cells produce a more vigorous hyperacute rejection than thymocytes, suggesting that B cells or macrophages may be the sensitizing agents. The accelerated rejection observed has the characteristics of an immunoglobulin M antibody-mediated hyperacute rejection response with deposition of complement.

摘要

背景

子宫内胎儿接种异基因细胞可产生对实验性心脏同种异体移植的后续耐受性。我们试图将这一观察结果扩展到异种心脏移植模型。

方法

在子宫内生命的第10天,给Lewis大鼠胎儿接种金黄叙利亚仓鼠胸腺细胞(n = 5)或全脾细胞(n = 5)。预处理胎儿出生6周后,使用仓鼠供体进行异位心脏移植。分娩后3至4周,我们在子宫内接受过治疗的雌性Lewis大鼠中使用仓鼠供体进行异位心脏移植。

结果

子宫内用胸腺细胞或全脾细胞治疗的动物移植存活时间为3天,与未治疗的Lewis大鼠(n = 5)无差异(p =无显著性差异)。胎儿用胸腺细胞(n = 5)或全脾细胞(n = 4)治疗的母本Lewis大鼠,其异种心脏移植的存活时间明显缩短(范围为3至20小时;平均为15小时;p < 0.01;以及范围为5至15分钟;平均为10分钟;p < 0.01)。未进行子宫内接种的雌性Lewis大鼠(n = 5)的异种移植存活时间符合预期(3天)(p =无显著性差异)。超急性排斥移植的免疫组织化学染色显示免疫球蛋白M以及免疫球蛋白G和补体的沉积。在正常排斥的异种移植中,未检测到免疫球蛋白M。

结论

这些研究揭示了一个惊人的观察结果,即胎儿暴露于异种细胞会使母本大鼠致敏,而不像在同种异体移植模型中那样使胎儿大鼠产生耐受性。此外,全脾细胞比胸腺细胞产生更强烈的超急性排斥反应,表明B细胞或巨噬细胞可能是致敏剂。观察到的加速排斥反应具有免疫球蛋白M抗体介导的超急性排斥反应的特征,并伴有补体沉积。

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