首页> 外文期刊>The Journal of heart and lung transplantation: the official publication of the International Society for Heart Transplantation >Transbronchial human interleukin-10 gene transfer reduces acute inflammation associated with allograft rejection and intragraft interleukin-2 and tumor necrosis factor-a gene expression in a rat model of lung transplantation
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Transbronchial human interleukin-10 gene transfer reduces acute inflammation associated with allograft rejection and intragraft interleukin-2 and tumor necrosis factor-a gene expression in a rat model of lung transplantation

机译:经支气管人类白细胞介素10基因转移减少与肺移植大鼠模型中同种异体移植排斥相关的急性炎症和移植物中白细胞介素2和肿瘤坏死因子-a基因表达

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BACKGROUND: The ability to express genes with potential immunoregulatory capacity could reduce allograft rejection (AR). This study examined the effect of ex vivo lipid-mediated transbronchial human interleukin-10 (ML-10) gene transfer on AR and the intragraft cytokine profile in a rat model of lung transplantation.METHODS: Left single lung transplants were performed between a highly histoincompatible combination of inbred rats. The donor left lung was extracted and intrabronchially instilled with a plasmid encoding ML-10 (IL-10 group) or Escherichia coli /3-galactosidase (control group), mixed with a cationic lipid. At 3 and 6 days after transplantation, the degree of AR was graded histologically (stage 1-4) and several pathologic categories of inflammation were scored on a scale of 0 to 4 according to the percentage of involvement. Intragraft cytokine profile was examined by real-time reverse transcription polymerase chain reaction.RESULTS: The stage of AR (3.1+-0.4 vs 3.8+-0.4) and the pathologic scores for edema (2.3+-0.8 vs 3.2+-0.4), intraalveolar hemorrhage (0.3+-0.5 vs 2.2+-0.8), and necrosis (0.3+-0.5 vs 1.2+-0.4) in the IL-10 group were significantly decreased compared with the control group at Day 6. IL-2 and tumor necrosis factor-a messenger RNA expression levels on Day 3 were significantly decreased in the IL-10 group. CONCLUSIONS: Ex vivo lipid-mediated transbronchial ML-10 gene transfer attenuated acute inflammation associated with AR, which was related to decreased levels of proinflammatory cytokine gene expression in a rat model of lung transplantation.
机译:背景:表达具有潜在免疫调节能力的基因的能力可以减少同种异体移植排斥(AR)。这项研究检查了离体脂质介导的人支气管白细胞介素10(ML-10)基因转移对大鼠肺移植模型中AR和移植物中细胞因子谱的影响。方法:左单肺移植是在高度组织相容性之间进行的近交大鼠的组合。提取供体左肺,并与编码脂质的脂质混合,将其编码ML-10(IL-10组)或大肠杆菌/ 3-半乳糖苷酶(对照组)进行支气管内滴注。移植后第3天和第6天,对AR的程度进行组织学分级(1-4期),并根据受累百分比在0到4分之间对炎症的几个病理学类别进行评分。结果:AR分期(3.1 + -0.4 vs 3.8 + -0.4)和水肿的病理评分(2.3 + -0.8 vs 3.2 + -0.4),通过实时逆转录聚合酶链反应检查了移植物中的细胞因子谱。与第6天的对照组相比,IL-10组的牙槽内出血(0.3 + -0.5 vs 2.2 + -0.8)和坏死(0.3 + -0.5 vs 1.2 + -0.4)明显减少。 IL-10组中第3天的坏死因子-α信使RNA表达水平显着降低。结论:离体脂质介导的经支气管ML-10基因转移减轻了与AR相关的急性炎症,这与大鼠肺移植模型中促炎细胞因子基因表达水平降低有关。

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