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大鼠肝移植后用甘氨酸调节库普弗细胞与耗尽库普弗细胞的益处:对缺血再灌注损伤、凋亡性细胞死亡、移植物再生和存活的影响

Benefit of Kupffer cell modulation with glycine versus Kupffer cell depletion after liver transplantation in the rat: effects on postischemic reperfusion injury, apoptotic cell death graft regeneration and survival.

作者信息

Rentsch Markus, Puellmann Kerstin, Sirek Slawo, Iesalnieks Igors, Kienle Klaus, Mueller Thomas, Bolder Ulrich, Geissler Edward, Jauch Karl-Walter, Beham Alexander

机构信息

Department of Surgery, Ludwig-Maximilians University of Munich, Klinikum Grosshadern, Munich, Germany.

出版信息

Transpl Int. 2005 Sep;18(9):1079-89. doi: 10.1111/j.1432-2277.2005.00185.x.

Abstract

Inhibition or destruction of Kupffer cells (KC) may protect against ischemia-reperfusion (IR) induced primary graft nonfunction (PNF) in liver transplantation. Besides KC activation, PNF is characterized by microvascular perfusion failure, intrahepatic leukocyte accumulation, cell death and hepatocellular dysfunction. KCs can be inactivated by different agents including gadolinium chloride (GdCl3), methyl palmitate (MP) and glycine. The effects of three KC inactivators on IR-injury after rat liver transplantation were compared in the present study. Lewis liver donors were treated with GdCl3, MP, glycine or saline (control). Liver grafts were transplanted following 24 h storage (UW solution). KC populations and IR damage were assessed by histologic analysis, quantitative real-time polymerase chain reaction (RT-PCR) and intravital microscopy. The number of hepatic ED-1 positive macrophages was diminished after GdCl3 (114.8+/-4.4/mm2 liver tissue) and MP treatment (176.0+/-5.0), versus the glycine (263.9+/-5.5) and control (272.1+/-5.6) groups. All three treatment modalities downregulated phagocytic activity for latex particles, paralleled by reduced microvascular injury (acinar perfusion index, GdCl3: 0.75+/-0.03; MP: 0.83+/-.03; glycine: 0.84+/-0.03; 0.63+/-0.03). Quantitative RT-PCR revealed elevated myeloperoxidase mRNA after glycine versus GdCl3 and MP pretreatment (3.2- and 3.4-fold, P=0.011, respectively), without difference to controls (2.9-fold of glycine). TNFalpha-mRNA was reduced after glycine- (5.2-fold), GdCl3- (19.7-fold), MP-treatment (39.5-fold) compared with controls. However, profound prevention of intrahepatic cell death and liver graft failure was solely achieved with glycine preconditioning. Different than GdCl3 and MP, glycine modulates rather than destroys KCs. Glycine appears to preserve cell viability and to TNFalpha/leukocyte dependent organ regeneration capacity, which is related to increase graft survival following liver transplantation.

摘要

抑制或破坏库普弗细胞(KC)可能有助于预防肝移植中缺血再灌注(IR)诱导的原发性移植肝无功能(PNF)。除了KC激活外,PNF的特征还包括微血管灌注衰竭、肝内白细胞积聚、细胞死亡和肝细胞功能障碍。KC可被不同药物灭活,包括氯化钆(GdCl3)、棕榈酸甲酯(MP)和甘氨酸。本研究比较了三种KC灭活剂对大鼠肝移植后IR损伤的影响。Lewis肝供体分别用GdCl3、MP、甘氨酸或生理盐水(对照)处理。肝脏移植物在保存24小时(UW溶液)后进行移植。通过组织学分析、定量实时聚合酶链反应(RT-PCR)和活体显微镜检查评估KC群体和IR损伤。与甘氨酸组(263.9±5.5)和对照组(272.1±5.6)相比,GdCl3(114.8±4.4/mm2肝组织)和MP处理后肝内ED-1阳性巨噬细胞数量减少。所有三种治疗方式均下调了对乳胶颗粒的吞噬活性,同时微血管损伤减少(腺泡灌注指数,GdCl3:0.75±0.03;MP:0.83±0.03;甘氨酸:0.84±0.03;对照组:0.63±0.03)。定量RT-PCR显示,与GdCl3和MP预处理相比,甘氨酸预处理后髓过氧化物酶mRNA升高(分别为3.2倍和3.4倍,P=0.011),与对照组无差异(甘氨酸的2.9倍)。与对照组相比,甘氨酸(5.2倍)、GdCl3(19.7倍)、MP处理(39.5倍)后TNFα-mRNA降低。然而,只有甘氨酸预处理能有效预防肝内细胞死亡和肝移植失败。与GdCl3和MP不同,甘氨酸调节而非破坏KC。甘氨酸似乎能保持细胞活力和TNFα/白细胞依赖性器官再生能力,这与肝移植后移植物存活增加有关。

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