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肝移植后移植物内白细胞介素-15 mRNA表达增加。

Increased intragraft IL-15 mRNA expression after liver transplantation.

作者信息

Baan C C, Niesters H G, Metselaar H J, Mol W M, Loonen E H, Zondervan P E, Tilanus H W, IJzermans J M, Schalm S W, Weimar W

机构信息

Department of Internal Medicine, University Hospital Rotterdam-Dijkzigt, The Netherlands.

出版信息

Clin Transplant. 1998 Jun;12(3):212-8.

PMID:9642512
Abstract

To study T-cell/macrophage interactions at the molecular level in clinical allograft rejection, we measured intragraft mRNA expression of the T-cell derived cytokine IL-2 and the macrophage derived chemokine IL-15, a novel cytokine associated with T-cell activation, in post-transplant liver biopsies (n = 33) and in non-transplanted control liver tissue by reverse transcriptase-polymerase chain reaction (RT-PCR). We analyzed biopsies without evidence of rejection (n = 12), with spontaneously resolving histological rejection (n = 10), or with histological rejection accompanied with clinical rejection (n = 11) defined by rising serum bilirubin and aspartate amino transaminase levels. IL-15 mRNA expression was present in the majority of post-transplant liver biopsies (91%, 30/33) and was significantly upregulated as compared with non-transplanted liver tissue (p = 0.005). However, the increased intragraft IL-15 mRNA level was not indicative for rejection. In contrast to intragraft IL-15 mRNA expression, IL-2 mRNA transcription was measured in the minority of the post-transplant liver biopsies (15%, 5/33) and not detectable in control specimens. In addition, IL-2 mRNA was almost specifically measured in rejection biopsies concurrent with graft dysfunction (36%, 4/11 versus 1/22 without clinical rejection; p = 0.03). No relation between intragraft IL-2 and IL-15 mRNA expression was found. The IL-15 mRNA expression levels were not higher in the IL-2 negative rejections compared with those in IL-2 positive rejections. To conclude, in contrast to IL-2, the function of IL-15 in T-cell mediated rejection remains unclear. The overall high IL-15 mRNA levels in sites of immune responses suggests that the macrophage-derived mediator IL-15 is involved in a constant flow of T-cells from the circulation into the graft.

摘要

为了在临床同种异体移植排斥反应中从分子水平研究T细胞与巨噬细胞的相互作用,我们通过逆转录聚合酶链反应(RT-PCR),检测了移植后肝活检组织(n = 33)和未移植对照肝组织中T细胞源性细胞因子白细胞介素-2(IL-2)以及巨噬细胞源性趋化因子白细胞介素-15(IL-15,一种与T细胞激活相关的新型细胞因子)的移植物内mRNA表达。我们分析了无排斥反应证据的活检组织(n = 12)、自发缓解组织学排斥反应的活检组织(n = 10)或伴有临床排斥反应(根据血清胆红素和天冬氨酸转氨酶水平升高定义)的组织学排斥反应的活检组织(n = 11)。IL-15 mRNA表达存在于大多数移植后肝活检组织中(91%,30/33),与未移植肝组织相比显著上调(p = 0.005)。然而,移植物内IL-15 mRNA水平升高并不提示排斥反应。与移植物内IL-15 mRNA表达相反,IL-2 mRNA转录在少数移植后肝活检组织中检测到(15%,5/33),在对照标本中未检测到。此外,IL-2 mRNA几乎仅在伴有移植物功能障碍的排斥反应活检组织中检测到(36%,4/11,而无临床排斥反应的为1/22;p = 0.03)。未发现移植物内IL-2和IL-15 mRNA表达之间存在关联。与IL-2阳性排斥反应相比,IL-2阴性排斥反应中IL-15 mRNA表达水平并不更高。总之,与IL-2不同,IL-15在T细胞介导的排斥反应中的作用仍不清楚。免疫反应部位总体较高的IL-15 mRNA水平表明,巨噬细胞源性介质IL-15参与了T细胞从循环系统持续流入移植物的过程。

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