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新生小鼠皮肤同种异体移植物的免疫耐受行为

Tolerogenic behavior of skin allografts from neonatal mice.

作者信息

Markees T G, De Fazio S R, Gozzo J J

机构信息

Bouvé College of Pharmacy and Health Sciences, Northeastern University, Boston, Massachusetts 02115.

出版信息

Transplantation. 1994 Nov 15;58(9):1008-14. doi: 10.1097/00007890-199411150-00006.

Abstract

Neonatal skin allografts can be tolerogenic when transplanted to appropriately immunosuppressed hosts. Single grafts of neonatal skin survive longer than adult skin grafts when recipients are treated with antilymphocyte serum (ALS) and donor bone marrow cells (BMC). Neonatal skin grafts can also prolong the survival of adult grafts of the same donor strain simultaneously cotransplanted with the neonatal grafts. To probe the mechanisms involved in this cotransplantation phenomenon, we delayed placement of the neonatal cotransplants relative to grafting with adult skin. Neonatal allografts placed either 7-9 days or 14 days after grafting with adult skin significantly prolonged adult graft survival in mice treated with ALS and BMC. However, day 0-placed neonatal cotransplants must remain on the recipient for > 2 weeks to prolong adult graft survival. Removal of cotransplants from ALS- and BMC-treated recipients after 7 or 14 days abrogated the cotransplantation effect. If left in place until day 21, neonatal cotransplants could significantly prolong adult graft survival, but did not induce the long-term graft survival observed in approximately 50% of the recipients whose cotransplants were not removed. Cotransplant removal after 1 year did not affect subsequent adult graft survival. Additionally, cotransplants were removed from recipients either on day 14 or from long-term graft-bearing mice and retransplanted to other ALS/BMC-treated recipients. These retransplanted grafts were unable to prolong survival of adult grafts on the new recipients. After transplant, but not before transplant, cyclophosphamide treatment of recipients prevented expression of the cotransplant effect in ALS-treated mice. However, recipient splenectomy > or = 1 week before grafting did not interfere with the effect. These results reflect on the contributions of the donor tissue, and the recipients' response, to the tolerogenic signals that permit a neonatal cotransplant to prolong adult graft survival.

摘要

将新生儿皮肤同种异体移植物移植到经过适当免疫抑制的宿主时可具有致耐受性。当受体接受抗淋巴细胞血清(ALS)和供体骨髓细胞(BMC)治疗时,单次移植的新生儿皮肤比成人皮肤移植物存活时间更长。新生儿皮肤移植物还可延长与新生儿移植物同时共移植的同一供体品系成人移植物的存活时间。为探究这种共移植现象所涉及的机制,我们将新生儿共移植的时间相对于成人皮肤移植进行了延迟。在成人皮肤移植后7 - 9天或14天植入的新生儿同种异体移植物显著延长了接受ALS和BMC治疗的小鼠中成人移植物的存活时间。然而,在第0天植入的新生儿共移植移植物必须在受体身上保留超过2周才能延长成人移植物的存活时间。在7天或14天后从接受ALS和BMC治疗的受体身上移除共移植移植物会消除共移植效应。如果保留到第21天,新生儿共移植移植物可显著延长成人移植物的存活时间,但不会诱导在约50%未移除共移植移植物的受体中观察到的长期移植物存活。1年后移除共移植移植物不影响随后成人移植物的存活。此外,在第14天从受体身上或从长期带有移植物的小鼠身上移除共移植移植物,并将其重新移植到其他接受ALS/BMC治疗的受体身上。这些重新移植的移植物无法延长新受体身上成人移植物的存活时间。移植后而非移植前,对受体进行环磷酰胺治疗可阻止ALS治疗小鼠中共移植效应的表达。然而,在移植前≥1周对受体进行脾切除并不干扰该效应。这些结果反映了供体组织和受体反应对允许新生儿共移植延长成人移植物存活的致耐受性信号的贡献。

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