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Cell therapy with a tissue-engineered kidney reduces the multiple-organ consequences of septic shock

 

作者: H. Humes,   Deborah Buffington,   Liandi Lou,   Simin Abrishami,   Min Wang,   Jun Xia,   William Fissell,  

 

期刊: Critical Care Medicine  (OVID Available online 2003)
卷期: Volume 31, issue 10  

页码: 2421-2428

 

ISSN:0090-3493

 

年代: 2003

 

出版商: OVID

 

关键词: cell therapy;acute renal failure;bioartificial organ;cytokines

 

数据来源: OVID

 

摘要:

ObjectiveGram-negative septic shock has a clinical mortality rate approaching 50%. The cause of death is secondary to a systemic inflammatory response syndrome with resulting cardiovascular collapse, ischemic damage to vital organs, and multiple-organ systems failure. Renal tubule cell injury occurs early in septic shock but is not clinically appreciated. Since renal tubule cells appear to play a critical role in the immunoregulation of stress states, renal cell therapy during septic shock may alter the detrimental multiple-organ consequences of systemic Gram-negative infection. The development of a tissue-engineered bioartificial kidney consisting of a conventional hemofiltration cartridge in series with a renal tubule assist device (RAD) containing 109renal proximal tubule cells may be a new therapeutic approach to this clinical disorder.DesignLaboratory study.SettingUniversity medical school.SubjectsPigs weighing 30–35 kg.InterventionsTo assess the effect of the bioartificial kidney and the RAD in septic shock, pigs were administered 30 × 1010bacteria/kg body weight ofEscherichia coliinto the peritoneal cavity and within 1 hr were immediately placed in a continuous venovenous hemofiltration extracorporeal circuit with either a sham RAD without cells or a RAD with cells.Measurements and Main ResultsIn this animal model, septic shock resulted within hours in acute tubule necrosis in the kidneys of all animals. Renal cell therapy resulted in significantly higher cardiac outputs and renal blood flow rates in treated animals compared with sham controls. RAD treatment also was associated with significantly lower plasma circulating concentrations of interleukin-6 and interferon-&ggr; compared with sham-treated animals. IL-6 release rates from peripheral blood mononuclear cells isolated from RAD-treated animals were significantly higher after endotoxin stimulation than those isolated from control animals. These physiologic and molecular alterations were associated with nearly a doubling of the average survival time in the RAD-treated group compared with the sham control group.ConclusionThese results demonstrate that renal cell therapy ameliorates cardiac and vascular dysfunction, alters systemic cytokine abnormalities, and improves survival time in a large animal model of Gram-negative septic shock. A cell therapeutic approach with a tissue-engineered bioartificial kidney may be a new treatment modality for this current unmet medical need.

 

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