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肾移植排斥反应的早期过程:确定排斥反应开始的时间。

The early course of kidney allograft rejection: defining the time when rejection begins.

作者信息

Einecke G, Mengel M, Hidalgo L, Allanach K, Famulski K S, Halloran P F

机构信息

Department of Medicine, Division of Nephrology and Transplantation Immunology, University of Alberta, Edmonton, Alberta, Canada.

出版信息

Am J Transplant. 2009 Mar;9(3):483-93. doi: 10.1111/j.1600-6143.2008.02546.x.

DOI:10.1111/j.1600-6143.2008.02546.x
PMID:19260832
Abstract

We studied the early events in mouse kidney allografts and isografts to define when allorecognition begins and when alloimmune tissue injury begins. Allografts but not isografts showed T-cell infiltration in perivascular areas from day 1, but tubulitis and arteritis did not develop until day 7. Flow cytometry confirmed the early allospecific CD3(+)CD8(+) T-cell infiltrate. At day 1, both allografts and isografts showed extensive transcriptome changes, reflecting the response to surgery, but only allografts showed expression of interferon-gamma (IFN-gamma)-inducible transcripts and T-cell-associated transcripts. Although the number of CD68(+) myeloid cell numbers did not increase in day 1 isografts or allografts, mRNA expression for myeloid markers was increased in isografts and allografts, suggesting activation of resident cells of the macrophage-dendritic cell series (MMDCs) in response to injury, followed by increased CD68(+) cell numbers from day 2. By day 3, an interstitial T-cell and MMDC infiltrate was established in allografts, corresponding with the emergence of allospecific tissue injury, as reflected by decreased parenchymal transcripts. Thus, in renal allografts, allorecognition by T cells occurs in perivascular sites by day 1, but alloimmune parenchymal damage begins at day 3, coinciding with the emergence of the interstitial T-cell-MMDC infiltrate.

摘要

我们研究了小鼠肾同种异体移植和同基因移植的早期事件,以确定异体识别何时开始以及同种异体免疫组织损伤何时开始。从第1天起,同种异体移植而非同基因移植在血管周围区域出现T细胞浸润,但直到第7天才出现肾小管炎和动脉炎。流式细胞术证实了早期同种异体特异性CD3(+)CD8(+) T细胞浸润。在第1天,同种异体移植和同基因移植均表现出广泛的转录组变化,这反映了对手术的反应,但只有同种异体移植表现出干扰素-γ(IFN-γ)诱导转录本和T细胞相关转录本的表达。尽管在第1天同基因移植和同种异体移植中CD68(+)髓样细胞数量均未增加,但同基因移植和同种异体移植中髓样标志物的mRNA表达均增加,这表明巨噬细胞-树突状细胞系列(MMDCs)的驻留细胞因损伤而被激活,随后从第2天起CD68(+)细胞数量增加。到第3天,同种异体移植中出现了间质T细胞和MMDC浸润,这与同种异体特异性组织损伤的出现相对应,表现为实质转录本减少。因此,在肾同种异体移植中,T细胞的异体识别在第1天就在血管周围部位发生,但同种异体免疫实质损伤在第3天开始,与间质T细胞-MMDC浸润的出现同时发生。

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