Differentiation Between Vascularized Composite Allograft Acute Skin Rejection and Delayed Type Hypersensitivity Reactions Based on Cytokine Analysis

D. Wolfram, H. Hackl, N. Eberhart, T. Hautz, R. Starzl, Nikolaus Thuille, Tanja Wachter, B. Zelger, G. Pierer, S. Schneeberger
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Abstract

Background: Skin rejection in vascularized composite allotransplantation is a major hurdle for wider clinical adoption in VCA. Histopathological alterations during acute skin rejection mimic inflammatory skin processes and are difficult to differentiate. The aim of this study was to identify protein expression patterns characteristic for acute skin rejection in reference to inflammatory skin processes, such as delayed type hypersensitivity reactions. Methods: Limb transplantations were performed using a Brown-Norway to Lewis rat allotransplant model. For the induction of skin inflammation a contact hypersensitivity (CHS) and delayed type hypersensitivity (DTH) model in Lewis rats were established. CHS and DTH result in skin irritation and swelling comparable to grade I-II rejection in our rat allotransplant model. While the DTH reaction is limited to the plantar skin, the CHS model allows for comparison with rejection also in hairy skin. Skin biopsies were taken at defined time points, where a histologically identical inflammatory response in all study groups was present. Protein levels of 14 inflammatory cytokines were assessed by Luminex™. Results: Based on the multivariate linear discriminant analysis, IL-12p70 and TNF-α were the major discriminators between skin rejection and inflammatory skin reactions. Principal component analysis identified IL-1α, GM-CSF, IL-6 and IL-18 as key drivers of rejection at this time point. Conclusion: The novel diagnostic platform enables for early and specific diagnosis of rejection and differentiation toward inflammatory skin diseases in this transplant model.
基于细胞因子分析的血管化复合同种异体移植急性皮肤排斥反应与延迟型超敏反应的鉴别
背景:血管化复合异体移植的皮肤排斥反应是VCA临床应用的主要障碍。急性皮肤排斥反应期间的组织病理学改变与皮肤炎症过程相似,难以区分。本研究的目的是确定炎症性皮肤过程(如延迟型超敏反应)中急性皮肤排斥反应的蛋白质表达模式。方法:采用Brown-Norway - Lewis大鼠同种异体移植模型进行肢体移植。为了诱导皮肤炎症,建立了Lewis大鼠接触性超敏反应(CHS)和延迟型超敏反应(DTH)模型。在我们的大鼠同种异体移植模型中,CHS和DTH导致皮肤刺激和肿胀,与I-II级排斥反应相当。虽然DTH反应仅限于足底皮肤,但CHS模型允许与毛皮肤的排斥反应进行比较。在规定的时间点进行皮肤活检,在所有研究组中存在组织学上相同的炎症反应。采用Luminex™检测14种炎性细胞因子的蛋白水平。结果:基于多元线性判别分析,IL-12p70和TNF-α是皮肤排斥反应与皮肤炎症反应的主要判别因子。主成分分析发现,IL-1α、GM-CSF、IL-6和IL-18是该时间点排斥反应的关键驱动因素。结论:新的诊断平台能够在移植模型中对排斥反应进行早期特异性诊断,并对炎症性皮肤病进行鉴别。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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