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首页> 外文期刊>Clinical transplantation. >Cytokine mRNA expression in chronically rejected human renal allografts.
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Cytokine mRNA expression in chronically rejected human renal allografts.

机译:慢性排斥的人类肾脏同种异体移植物中的细胞因子mRNA表达。

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Nocera A, Tagliamacco A, De Palma R, Del Galdo F, Ferrante A, Fontana I, Barocci S, Ginevri F, Rolla D, Ravetti JL, Valente U. Cytokine mRNA expression in chronically rejected human renal allografts. Clin Transplant 2004 DOI: 10.1111/j.1399-0012.2004.00227.x Copyright Blackwell Munksgaard, 2004Abstract: Although both immunologic and non-immunologic components may cause kidney allograft chronic rejection (KGCR), also referred to as chronic allograft nephropathy (CAN), its pathogenesis is largely not yet understood. To explore relevant immunologic mechanisms occurring in KGCR, we have analyzed in surgically removed KG the transcription of the following cytokine and apoptotic molecule genes: interleukin (IL)-2, IL-3, IL-4, IL-5, IL-6, IL-10, tumor necrosis factor (TNF)-alpha, IFN-gamma, FAS, and FAS-L. Semiquantitative RT-PCR was used and KG explants were obtained from two groups of transplanted patients. Group 1 was represented by CR/CAN KG, removed for: (a) superimposed symptoms of acute lesions (SAL) due to tapering or suspension of immunosuppression (subgroup 1a, eight cases); (b) causes other than SAL (two cases, subgroup 1b). Group 2 comprised explanted kidneys with no CR/CAN (three cases - vascular thrombosis, intrarenal hemorrhage and vascular thrombosis). The results showed that in group 1 IL- 6 was detectable in seven of 10, IL-10 in six of 10, IFN-gamma in five of 10, and IL-3 in four of 10 cases with a variable pattern of reciprocal association. IL-2 and TNF-alpha were represented in one of 10 cases only. Particularly, in the subgroup 1b IL-10 was never detected. Among the most represented cytokines of group 1, IL-10 as well as IL-3 were never found in group 2. The peculiar expression of IL-10 and IL-3 and partially IL-6 seems to support the hypothesis that a Th2 pattern predominantly characterizes KGCR, thus indicating that Th2 cytokines, likely produced by different intragraft cell types including T cells, macrophages and natural killer (NK) cells, may represent an important component in the pathogenesis of this process. Moreover, IL-10 seems to exquisitely characterize a group of CR/CAN kidney grafts more prone to immunologic assaults.
机译:Nocera A,Tagliamacco A,De Palma R,Del Galdo F,Ferrante A,Fontana I,Barocci S,Ginevri F,Rolla D,Ravetti JL,ValenteU。在慢性排斥的人肾移植物中的细胞因子mRNA表达。临床移植2004年DOI:10.1111 / j.1399-0012.2004.00227.x版权所有Blackwell Munksgaard,2004年摘要:尽管免疫和非免疫成分均可能导致肾脏同种异体移植慢性排斥反应(KGCR),也称为慢性同种异体移植肾病(CAN) ,其发病机理在很大程度上尚不清楚。为了探讨发生在KGCR中的相关免疫学机制,我们在外科切除的KG中分析了以下细胞因子和凋亡分子基因的转录:白介素(IL)-2,IL-3,IL-4,IL-5,IL-6, IL-10,肿瘤坏死因子(TNF)-α,IFN-γ,FAS和FAS-L。使用半定量RT-PCR,从两组移植患者中获得KG外植体。第1组以CR / CAN KG代表,因以下原因而被移除:(a)由于免疫抑制作用的减弱或中止而导致的急性损伤(SAL)的叠加症状(亚组1a,八例); (b)SAL以外的原因(两种情况,子组1b)。第2组包括没有CR / CAN的移植肾脏(3例-血管血栓形成,肾内出血和血管血栓形成)。结果显示,在第1组中,具有可变的相互联系模式的患者中,有10例中有7例,6例中有10例IL-10、10例中有5例检测到IFN-γ,10例中有4例检测到IL-3。 IL-2和TNF-α仅代表10例。特别地,在亚组1b中从未检测到IL-10。在第1组中最具代表性的细胞因子中,第2组中从未发现IL-10和IL-3。IL-10和IL-3和部分IL-6的特殊表达似乎支持了Th2模式的假设。 KGCR的主要特征,因此表明可能由不同的移植物内细胞类型(包括T细胞,巨噬细胞和自然杀伤(NK)细胞)产生的Th2细胞因子可能代表了这一过程的发病机理。而且,IL-10似乎可以很好地表征一组CR / CAN肾移植物,更易于发生免疫攻击。

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