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输血对大鼠心脏同种异体移植影响的遗传学研究

Genetics of the blood transfusion effect on heart allografts in rats.

作者信息

Soulillou J P, Blandin F, Günther E, Lemoine V

出版信息

Transplantation. 1984 Jul;38(1):63-7. doi: 10.1097/00007890-198407000-00015.

Abstract

Working with the recently available recombinant haplotypes of the rat major histocompatibility complex (MHC)--RT1, we investigated the effect of various types of blood transfusion (BT) on allograft prolongation, including blood identical for the whole RT1 haplotype with that of the donor or for only a part of it. One or two milliliters of donor blood significantly prolonged graft survival in the (LEW X BN)F1----LEW or the LEW X 1W----LEW X 1A combination. The optimal regimen consisted of two BTs given 15 and 7 days prior to grafting; BTs given at day -30 were ineffective. A BT given on the day of the operation was effective, but sequential BTs after grafting did not further increase graft survival. In the (LEW X BN)F1----LEW combination, blood from congenic LEW X 1N rats significantly prolonged graft survival, but third-party BTs were ineffective or had only a borderline effect when transfused (1 ml, 8 times) within the three months before transplantation. This showed the major role of the RT1 system as well as the specificity of the model. Although the survival of LEW X 1A heart grafts transplanted into LEW X 1W recipients could not be significantly prolonged by donor blood, with the reverse--and "weaker"--combination (LEW X 1W----LEW X 1A), 2 ml of donor blood led, in all cases, to greater than 100 days graft survival. In this last combination, third-party BT (LEW X 1N) was again totally ineffective. Blood from RT1-recombinant rats was used to test the role of the respective RT1.A, B, and C regions, in the enhancing effect. BTs from LEW X 1AR2 or LEW X 1WR2 recombinants--sharing, respectively, RT1.C and RT1.A with the graft donor--were only moderately effective, as compared with BTs from the graft donor. On the other hand, LEW X 1WR1 BTs--sharing the RT1.A and RT1.B regions with the graft donor--had a much more powerful effect on heart survival. The results strongly suggest that the RT1.B region (coding for Ia-like antigens) must be shared by the graft and blood donor in order to mediate a significant graft prolongation.

摘要

利用最近可得的大鼠主要组织相容性复合体(MHC)——RT1的重组单倍型,我们研究了不同类型输血(BT)对同种异体移植延长的影响,包括与供体整个RT1单倍型相同或仅部分相同的血液。1或2毫升供体血液显著延长了(LEW×BN)F1——LEW或LEW×1W——LEW×1A组合中的移植物存活时间。最佳方案是在移植前15天和7天进行两次输血;在第-30天进行的输血无效。在手术当天进行的输血有效,但移植后连续输血并未进一步提高移植物存活率。在(LEW×BN)F1——LEW组合中,同源LEW×1N大鼠的血液显著延长了移植物存活时间,但在移植前三个月内输注(1毫升,8次)第三方输血无效或仅有边缘效应。这显示了RT1系统的主要作用以及该模型的特异性。尽管将LEW×1A心脏移植物移植到LEW×1W受体中时,供体血液不能显著延长其存活时间,但在反向且“较弱”的组合(LEW×1W——LEW×1A)中,2毫升供体血液在所有情况下都能使移植物存活超过100天。在最后这种组合中,第三方输血(LEW×1N)再次完全无效。来自RT1重组大鼠的血液用于测试各自的RT1.A、B和C区域在增强作用中的作用。与来自移植物供体的输血相比,分别与移植物供体共享RT1.C和RT1.A的LEW×1AR2或LEW×1WR2重组体的输血效果仅为中等。另一方面,与移植物供体共享RT1.A和RT1.B区域的LEW×1WR

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