Literature DB >> 10528603

Multiple organ dysfunction after remote circulatory arrest: common pathway of radical oxygen species?

A A Weinbroum1, E Hochhauser, V Rudick, Y Kluger, E Karchevsky, E Graf, B A Vidne.   

Abstract

OBJECTIVES: Cardiovascular, respiratory, and vascular dysfunction can follow trauma-induced no-flow-reflow states: hemorrhage, blunt trauma, or neurogenic shock. Liver ischemia-reperfusion (IR) induces remote lung damage by means of xanthine oxidase (XO) pro-oxidant activity. This damage was not proven in the heart, neither was the independent role of radical oxygen species (ROS) established in such cases. We investigated whether multiple organ dysfunction after a trauma-like IR is XO and ROS related and whether clinically used ROS scavengers could be beneficial.
METHODS: A controlled, randomized trial in which isolated rat livers, hearts, lungs, and aortic rings were perfused with Krebs-Henseleit solutions. After stabilization, livers were either perfused or made ischemic (2 hours). Then, pairs of liver plus heart, lung, or ring were reperfused in series (15 minutes), and then the second organ circulated alone for 45 minutes. Remote organ protection against the pro-oxidant hepatic-induced toxicity was evaluated by using allopurinol (1 mmol/L, heart), mannitol (0.25 g/kg, lung), or methylene blue (40 mg/kg, ring).
RESULTS: IR liver effluents typically contained high lactate dehydrogenase, XO, and uric acid concentrations compared with control organs. IR was associated with doubled lung peak inspiratory pressure and reduced static compliance. Myocardial velocity of contraction and relaxation decreased by one third of baseline, and rings contracted abnormally and responded inadequately to phenylephrine. Wet-weight to dry-weight ratios in the remote organs increased as well. Most remote reperfusion injuries were attenuated by the drugs.
CONCLUSION: Liver no-flow-reflow directly induces myocardial, pulmonary, and vascular dysfunction. These are likely mediated by XO and ROS. The tested drugs protected against these pro-oxidants, even in the presence of circulating XO.

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Year:  1999        PMID: 10528603     DOI: 10.1097/00005373-199910000-00013

Source DB:  PubMed          Journal:  J Trauma        ISSN: 0022-5282


  14 in total

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Review 2.  The effect of antioxidant supplementation on bacterial translocation after intestinal ischemia and reperfusion.

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3.  Mannitol attenuates acute lung injury induced by infrarenal aortic occlusion-reperfusion in rats.

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4.  Effects of vasoactive substances released from ischemic reperfused liver on the isolated rat heart.

Authors:  E Hochhauser; I Alterman; A Weinbroum; Y Barak; D Harell; A Raz; A Erman; B Vidne
Journal:  Exp Clin Cardiol       Date:  2001

5.  Mesenteric artery clamping/unclamping-induced acute lung injury is attenuated by N-methyl-D-aspartate antagonist dextromethorphan.

Authors:  R Ben-Abraham; M Guttman; R Flaishon; N Marouani; D Niv; Avi A Weinbroum
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6.  Relationship between oxidative stress in muscle tissue and weight-lifting-induced muscle damage.

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7.  Combined early fluid resuscitation and hydrogen inhalation attenuates lung and intestine injury.

Authors:  Wei Liu; Li-Ping Shan; Xue-Song Dong; Xiao-Wei Liu; Tao Ma; Zhi Liu
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8.  Renal oxidative stress following CO2 pneumoperitoneum-like conditions.

Authors:  Wisam Khoury; Letizia Schreiber; Amir Szold; Joseph M Klausner; Avi A Wienbroum
Journal:  Surg Endosc       Date:  2008-07-16       Impact factor: 4.584

9.  Mannitol prevents acute lung injury after pancreas ischemia-reperfusion: a dose-response, ex vivo study.

Authors:  Avi A Weinbroum
Journal:  Lung       Date:  2009-06-17       Impact factor: 2.584

10.  Carbon dioxide pneumoperitoneum-related liver injury is pressure dependent: A study in an isolated-perfused organ model.

Authors:  Amir Szold; Avi A Weinbroum
Journal:  Surg Endosc       Date:  2007-07-28       Impact factor: 4.584

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