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1型糖尿病受体肝脏中移植胰岛原位的供体来源及状况鉴定

Identification of Donor Origin and Condition of Transplanted Islets In Situ in the Liver of a Type 1 Diabetic Recipient.

作者信息

van der Torren Cornelis R, Suwandi Jessica S, Lee DaHae, Van't Wout Ernst-Jan T, Duinkerken Gaby, Swings Godelieve, Mulder Arend, Claas Frans H J, Ling Zhidong, Gillard Pieter, Keymeulen Bart, In't Veld Peter, Roep Bart O

出版信息

Cell Transplant. 2017 Jan 24;26(1):1-9. doi: 10.3727/096368916X693437. Epub 2016 Oct 10.

Abstract

Transplantation of islet allografts into type 1 diabetic recipients usually requires multiple pancreas donors to achieve insulin independence. This adds to the challenges of immunological monitoring of islet transplantation currently relying on surrogate immune markers in peripheral blood. We investigated donor origin and infiltration of islets transplanted in the liver of a T1D patient who died of hemorrhagic stroke 4 months after successful transplantation with two intraportal islet grafts combining six donors. Immunohistological staining for donor HLA using a unique panel of human monoclonal HLA-specific alloantibodies was performed on liver cryosections after validation on cryopreserved kidney, liver, and pancreas and compared with auto- and alloreactive T-cell immunity in peripheral blood. HLA-specific staining intensity and signal-to-noise ratio varied between tissues from very strong on kidney glomeruli, less in liver, kidney tubuli, and endocrine pancreas to least in exocrine pancreas, complicating the staining of inflamed islets in an HLA-disparate liver. Nonetheless, five islets from different liver lobes could be attributed to donors 1, 2, and 5 by staining patterns with multiple HLA types. All islets showed infiltration with CD8+ cytotoxic T cells that was mirrored by progressive alloreactive responses in peripheral blood mononuclear cells (PBMCs) to donors 1, 2, and 5 after transplantation. Stably low rates of peripheral islet autoreactive T-cell responses after islet infusion fit with a complete HLA mismatch between grafts and recipient and exclude the possibility that the islet-infiltrating CD8 T cells were autoreactive. HLA-specific immunohistochemistry can identify donor origin in situ and differentiate graft dysfunction and immunological destruction.

摘要

将胰岛同种异体移植物移植到1型糖尿病受者体内通常需要多个胰腺供体才能实现胰岛素自主分泌。这增加了目前依赖外周血替代免疫标志物进行胰岛移植免疫监测的挑战。我们研究了一名1型糖尿病患者的胰岛供体来源及移植情况,该患者在成功移植两个门静脉内胰岛移植物(合并六个供体)4个月后死于出血性中风,胰岛被移植到肝脏中。在对冷冻保存的肾脏、肝脏和胰腺进行验证后,使用一组独特的人源单克隆HLA特异性同种抗体对肝脏冰冻切片进行供体HLA免疫组织化学染色,并与外周血中的自身反应性和同种反应性T细胞免疫进行比较。HLA特异性染色强度和信噪比在不同组织之间有所不同,在肾小球上非常强,在肝脏、肾小管和内分泌胰腺中较弱,在外分泌胰腺中最弱,这使得在HLA不匹配的肝脏中对炎症胰岛进行染色变得复杂。尽管如此,通过多种HLA类型的染色模式,可以将来自不同肝叶的五个胰岛归属于供体1、2和5。所有胰岛均显示有CD8 + 细胞毒性T细胞浸润,移植后外周血单核细胞(PBMC)对供体1、2和5的同种反应性反应逐渐增强,这与胰岛浸润情况相符。胰岛输注后外周胰岛自身反应性T细胞反应率持续较低,这与移植物和受体之间完全HLA不匹配相符,并排除了胰岛浸润性CD8 T细胞为自身反应性的可能性。HLA特异性免疫组织化学可以原位识别供体来源,并区分移植物功能障碍和免疫破坏。

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Transplanted human pancreatic islets after long-term insulin independence.移植的人胰岛后长期胰岛素依赖。
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Histologic graft assessment after clinical islet transplantation.临床胰岛移植后的组织学移植物评估。
Transplantation. 2009 Dec 15;88(11):1286-93. doi: 10.1097/TP.0b013e3181bc06b0.

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