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首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Oxidative DNA damage after transplantation of the liver and small intestine in pigs.
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Oxidative DNA damage after transplantation of the liver and small intestine in pigs.

机译:猪肝脏和小肠移植后的氧化DNA损伤。

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Oxidative damage is thought to play an important role in ischemia/reperfusion injury, including the outcome of transplantation of the liver and intestine. We have investigated oxidative DNA damage after combined transplantation of the liver and small intestine in 5 pigs. DNA damage was estimated from the urinary excretion of the repair product 8-oxo-7,8-dihydro-2'-deoxyguanosine (8-oxodG). In the first 1-3 hr after reperfusion of the grafts, 8-oxodG excretion was increased 2.9-fold (1.7-4.1; 95% confidence intervals; P < 0.05). A control experiment included sham surgery with clamping of the suprarenal inferior caval vein in 2 pigs during steady state infusion of 8-oxodG. While the caval vein was clamped, the urinary excretion of 8-oxodG was almost blocked, whereas after removal of the clamp, the excretion returned to and did not exceed the preclamp levels. In a separate experiment with 2 pigs, the elimination of injected 8-oxodG was shown to adhere to first-order kinetics with a clearance and a terminal elimination half-life of approximately 4 ml min-1 kg-1 and 2 1/2 hr, respectively. The injected dose was completely excreted into the urine within 4 hr. It is concluded that substantial oxidative damage to DNA results from reperfusion of transplanted small intestine and liver in pigs, as estimated from the readily excreted repair product 8-oxodG.
机译:氧化损伤被认为在缺血/再灌注损伤中起重要作用,包括肝脏和肠移植的结果。我们研究了肝和小肠联合移植后在5头猪中的氧化DNA损伤。 DNA损伤是由修复产物8-oxo-7,8-dihydro-2'-deoxyguanosine(8-oxodG)的尿排泄估计的。在移植物再灌注后的最初1-3小时内,8-oxodG的排泄增加了2.9倍(1.7-4.1; 95%的置信区间; P <0.05)。对照实验包括假手术,在稳定输注8-oxodG的过程中,对2头猪的肾上下腔静脉进行了夹持。夹住腔静脉时,尿中的8-oxodG排泄几乎被阻塞,而移开夹后,排泄物恢复到并且未超过预夹水平。在另一只2头猪的实验中,注射的8-oxodG的消除显示出符合一级动力学的规律,清除和最终消除半衰期约为4 ml min-1 kg-1和2 1/2 hr。 , 分别。注射剂量在4小时内完全排入尿液。结论是,根据容易排泄的修复产物8-oxodG估计,对猪的小肠和肝脏的再灌注会导致对DNA的大量氧化损伤。

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