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首页> 外文期刊>Nephron >The Synthesis by Fine-Needle Aspiration Biopsy Cultures of IL-7, IL-16 and IL-18 Is Significantly Associated with Acute Rejection in Kidney Transplants.
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The Synthesis by Fine-Needle Aspiration Biopsy Cultures of IL-7, IL-16 and IL-18 Is Significantly Associated with Acute Rejection in Kidney Transplants.

机译:IL-7,IL-16和IL-18的细针穿刺活检培养物的合成与肾脏移植物中的急性排斥反应显着相关。

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Background: T-cell activation, the key event in the development of acute allograft rejection, depends on co-stimulatory signals delivered by antigen-presenting cells (APC). APC-derived cytokines may provide co-stimulation and modulate alloimmune reaction. We have studied cytokine synthesis by fine-needle aspiration biopsy (FNAB) culture and we found significant differences for interleukin (IL)-2, IL-6, IL-10, M-CSF and IL-1ra on comparing acute rejection versus stable kidney transplant patients. We report our findings on FNAB cultures synthesis of IL-7, IL-15, IL-16, IL-17, IL-18 and RANTES (regulated upon activation, normal T-cell expressed and secreted), all potential modulators of anti-graft reaction. Patients and Methods: Kidney transplants (KTX) treated with CsA-AZA-Pred from the beginning, were divided into four groups. Group I: day 7 post-KTX, stable; II: day 7 post-KTX, 6.5 +/- 5.5 days before acute rejection; III: first day of acute rejection; IV: day 14 post-KTX, stable. Patients from I and IV remained rejection-free for the first 6 months, at least. All rejection episodes were confirmed by classical core renal biopsy. FNAB samples were cultured according to our published methodology and culture supernatants were collected at 48 h and analysed by ELISA for IL-7, IL-15, IL-16, IL-17, IL-18 and RANTES. Results: Group III synthesized significantly higher amounts of IL-7, IL-16 and IL-18 than stable patients (groups I and IV). RANTES production did not show significant differences among the four groups. We did not find any trace of IL-15. Conclusions: IL-18 may play the activation role that has been attributed to IL-12 which previously, we did not find to correlate significantly with acute rejection in KTX. IL-16 seems to play an activation role rather than an inhibition of anti-graft reaction. We confirm that RANTES is not significantly associated with acute rejection in KTX.
机译:背景:T细胞活化是急性同种异体移植排斥反应发展的关键事件,取决于抗原呈递细胞(APC)传递的共刺激信号。 APC衍生的细胞因子可能提供共刺激作用并调节同种免疫反应。我们已经通过细针穿刺活检(FNAB)培养研究了细胞因子的合成,并且在比较急性排斥反应和稳定肾脏方面发现白介素(IL)-2,IL-6,IL-10,M-CSF和IL-1ra有显着差异移植患者。我们报告了关于FNAB培养物IL-7,IL-15,IL-16,IL-17,IL-18和RANTES合成的发现(激活后调节,正常T细胞表达和分泌),所有潜在的调节剂接枝反应。患者和方法:从一开始就用CsA-AZA-Pred治疗肾脏移植(KTX),分为四组。第一组:KTX后第7天,情况稳定; II:KTX后第7天,急性排斥反应前6.5 +/- 5.5天; III:急性排斥的第一天; IV:KTX后第14天稳定。来自I和IV的患者至少在最初的6个月内保持无排斥。所有排斥反应均通过经典的核心肾活检证实。根据我们公开的方法培养FNAB样品,并在48 h收集培养上清液,并通过ELISA分析IL-7,IL-15,IL-16,IL-17,IL-18和RANTES。结果:III组合成的IL-7,IL-16和IL-18的数量明显高于稳定患者(I和IV组)。 RANTES生产在四组之间没有显示显着差异。我们没有发现任何IL-15痕迹。结论:IL-18可能起因于IL-12的激活作用,以前我们没有发现它与KTX的急性排斥反应显着相关。 IL-16似乎起激活作用而不是抑制抗移植物反应。我们确认RANTES与KTX的急性排斥反应没有显着相关。

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