首页> 外文期刊>Journal of the American Society of Nephrology: JASN >Bioartificial kidney ameliorates gram-negative bacteria-induced septic shock in uremic animals.
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Bioartificial kidney ameliorates gram-negative bacteria-induced septic shock in uremic animals.

机译:生物人工肾脏改善了尿毒症动物中革兰氏阴性细菌引起的败血性休克。

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摘要

The bioartificial kidney (BAK) consists of a conventional hemofiltration cartridge in series with a renal tubule assist device (RAD) containing 10(9) porcine renal proximal tubule cells. BAK replaces filtration, transport, and metabolic and endocrinologic activities of a kidney. Previous work in an acutely uremic dog model demonstrated that BAK ameliorated endotoxin (lipopolysaccharide [LPS])-induced hypotension and altered plasma cytokine levels. To further assess the role of BAK in sepsis in acute renal failure, dogs were nephrectomized and 48 h later administered intraperitoneally with 30 x 10(10) bacteria/kg of E. coli. One hour after bacterial administration, animals were placed in a continuous venovenous hemofiltration circuit with either a sham RAD without cells (n = 6) or a RAD with cells (n = 6). BP, cardiac output, heart rate, pulmonary capillary wedge pressure, and systemic vascular resistance were measured throughout the study. All animals tested were in renal failure, with blood urea nitrogen and serum creatinine concentrations greater than 60 and 6 mg/dl, respectively. RAD treatment maintained significantly better cardiovascular performance, as determined by arterial BP (P < 0.05) and cardiac output (P < 0.02), for longer periods than sham RAD therapy. Consistently, all sham RAD-treated animals, except one, expired within 2 to 9 h after bacterial administration, whereas all RAD-treated animals survived more than 10 h. Plasma levels of TNF-alpha, IL-10, and C-reactive protein (CRP) were measured during cell RAD and sham RAD treatment. IL-10 levels were significantly higher (P < 0.01) during the entire treatment interval in the RAD animals compared with sham controls. These data demonstrated in a pilot large animal experiment that the BAK with RAD altered plasma cytokine levels in acutely uremic animals with septic shock. This change was associated with improved cardiovascular performance and increased survival time. These results demonstrate that the addition of cell therapy to hemofiltration in an acutely uremic animal model with septic shock ameliorates cardiovascular dysfunction, alters systemic cytokine balance, and improves survival time.
机译:生物人工肾脏(BAK)由常规的血液滤过滤筒和与肾小管辅助装置(RAD)串联而成,该装置包含10(9)个猪肾近端小管细胞。 BAK替代肾脏的过滤,运输以及代谢和内分泌活动。先前在急性尿毒症狗模型中的工作表明,BAK改善了内毒素(脂多糖[LPS])诱导的低血压并改变了血浆细胞因子水平。为了进一步评估BAK在脓毒症在急性肾衰竭中的作用,将狗肾切除,并在48小时后腹膜内给予30 x 10(10)细菌/ kg大肠杆菌。细菌给药后一小时,将动物置于连续的静脉血液滤过回路中,该回路具有不带细胞的假RAD(n = 6)或带细胞的srad RAD(n = 6)。在整个研究过程中均测量了BP,心输出量,心率,肺毛细血管楔压和全身血管阻力。测试的所有动物均患有肾衰竭,血液尿素氮和血清肌酐浓度分别高于60和6 mg / dl。与假RAD治疗相比,根据动脉血压(P <0.05)和心输出量(P <0.02)确定,RAD治疗的心血管性能显着提高。一致地,除一只假手术外,所有假手术的RAD处理动物均在细菌施用后2至9小时内死亡,而所有RAD处理的动物均存活超过10小时。在细胞RAD和假RAD处理期间测量血浆TNF-α,IL-10和C反应蛋白(CRP)的水平。与假对照组相比,RAD动物在整个治疗期间的IL-10水平明显更高(P <0.01)。这些数据在大型动物实验中证明,带有RAD的BAK可以改变败血性休克的急性尿毒症动物的血浆细胞因子水平。这种变化与心血管功能的改善和生存时间的延长有关。这些结果表明,在患有败血性休克的急性尿毒症动物模型中,将细胞疗法添加到血液滤过中可改善心血管功能障碍,改变全身细胞因子平衡并延长生存时间。

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