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接受微血管化肢体移植的未受照射、环孢素处理大鼠的骨髓源性嵌合体:受体淋巴组织中供体来源树突状细胞的证据。

Bone marrow-derived chimerism in non-irradiated, cyclosporin-treated rats receiving microvascularized limb transplants: evidence for donor-derived dendritic cells in recipient lymphoid tissues.

作者信息

Talmor M, Steinman R M, Codner M A, Chen M, Harper A D, Witmer-Pack M D, Hoffman L A

机构信息

Laboratory of Cellular Physiology and Immunology, Rockefeller University, New York, USA.

出版信息

Immunology. 1995 Nov;86(3):448-55.

Abstract

Tolerance to donor transplantation antigens develops when recipients are made chimeric with donor bone marrow. To establish chimerism, the haemopoietic system of recipients typically is severely compromised. We report on a system in which chimerism develops without ablative therapies. Immunosuppression with cyclosporin A allowed the lower limb of a rat to be replaced by a microvascularized transplant from a fully allogeneic donor. Many donor-derived cells populated recipient lymph nodes and spleen, and most had the large size, irregular shape and strong major histocompatibility complex (MHC) class II expression that typify dendritic cells. Donor cells were not found in the macrophage-rich regions of lymphoid tissues, but instead occupied splenic white pulp and lymph node cortex. The donor cells were derived from radiosensitive marrow precursors, as chimerism was abolished if the grafted limb was irradiated, or if muscle and skin flaps devoid of bone were grafted. Donor cells were rare or not detectable in blood, thymus and liver. Whereas lymphoid chimerism was prominent following limb transfer, donor cells were not detected 1-2 weeks after an injection of two femur equivalents of a marrow suspension. We suggest that dendritic cells that undergo rapid turnover in lymphoid organs are replaced from allogeneic precursors in bone grafts. The combination of cyclosporin and vascularized bone provides a means for inducing chimerism in lymphoid tissues of non-irradiated recipients.

摘要

当受体与供体骨髓形成嵌合体时,会产生对供体移植抗原的耐受性。为了建立嵌合状态,受体的造血系统通常会受到严重损害。我们报道了一种无需进行清髓疗法即可形成嵌合状态的系统。用环孢素A进行免疫抑制,使得大鼠的下肢能够被来自完全异基因供体的微血管化移植组织所替代。许多供体来源的细胞定植于受体的淋巴结和脾脏,且大多数细胞具有典型树突状细胞的大尺寸、不规则形状和强烈的主要组织相容性复合体(MHC)II类表达。在富含巨噬细胞的淋巴组织区域未发现供体细胞,而是占据了脾脏白髓和淋巴结皮质。供体细胞来源于对辐射敏感的骨髓前体细胞,因为如果对接种的肢体进行照射,或者移植不含骨骼的肌肉和皮瓣,嵌合状态就会消失。在血液、胸腺和肝脏中,供体细胞很少见或无法检测到。虽然肢体移植后淋巴嵌合现象很明显,但在注射相当于两根股骨量的骨髓悬液1 - 2周后未检测到供体细胞。我们认为,在淋巴器官中快速更新的树突状细胞是由骨移植中的异基因前体细胞替代的。环孢素与血管化骨的结合为在未受照射的受体的淋巴组织中诱导嵌合状态提供了一种方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cb5c/1383950/1829aa8ae4a2/immunology00064-0128-a.jpg

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