Literature DB >> 9739056

Protective role of endogenous carbon monoxide in hepatic microcirculatory dysfunction after hemorrhagic shock in rats.

B H Pannen1, N Köhler, B Hole, M Bauer, M G Clemens, K K Geiger.   

Abstract

Maintenance of hepatic microcirculatory flow after ischemia of the liver is essential to prevent hepatic dysfunction. Thus, we determined the differential role of carbon monoxide (CO) and nitric oxide (NO) in the intrinsic control of sinusoidal perfusion, mitochondrial redox state, and bile production in the isolated perfused rat liver after hemorrhagic shock. Administration of tin protoporphyrin-IX (50 microM), a specific inhibitor of the CO generating enzyme heme oxygenase, caused a decrease in sinusoidal flow that was more pronounced after shock compared with sham shock, as determined by in situ epifluorescence microscopy. This was associated with a shift in hepatocellular redox potential to a more reduced state (increased fluorescence intensity of reduced pyridine nucleotides in hepatocytes, decreased acetoacetate/beta-hydroxybutyrate ratio in the perfusate) and a profound reduction in bile flow. In sharp contrast, the preferential inhibitor of the inducible isoform of NO synthase S-methylisothiourea sulfate (100 microM) did not affect sinusoidal flow, hepatic redox state, or function. This indicates that 1.) endogenously generated CO preserves sinusoidal perfusion after hemorrhagic shock, 2.) protection of the hepatic microcirculation by CO may serve to limit shock-induced liver dysfunction, and 3.) in contrast to CO, inducible NO synthase-derived NO is of only minor importance for the intrinsic control of hepatic perfusion and function under these conditions.

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Year:  1998        PMID: 9739056      PMCID: PMC509105          DOI: 10.1172/JCI3428

Source DB:  PubMed          Journal:  J Clin Invest        ISSN: 0021-9738            Impact factor:   14.808


  52 in total

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  25 in total

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Journal:  Intensive Care Med       Date:  2008-02-20       Impact factor: 17.440

Review 6.  Carbon monoxide in exhaled breath testing and therapeutics.

Authors:  Stefan W Ryter; Augustine M K Choi
Journal:  J Breath Res       Date:  2013-02-27       Impact factor: 3.262

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Authors:  Stefan W Ryter; Kevin C Ma; Augustine M K Choi
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8.  Carbon monoxide inhalation protects rat intestinal grafts from ischemia/reperfusion injury.

Authors:  Atsunori Nakao; Kei Kimizuka; Donna B Stolz; Joao Seda Neto; Takashi Kaizu; Augustine M K Choi; Takashi Uchiyama; Brian S Zuckerbraun; Michael A Nalesnik; Leo E Otterbein; Noriko Murase
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9.  Carbon monoxide protects against hemorrhagic shock and resuscitation-induced microcirculatory injury and tissue injury.

Authors:  Ibrahim Nassour; Benjamin Kautza; Mark Rubin; Daniel Escobar; Jason Luciano; Patricia Loughran; Hernando Gomez; Jeffrey Scott; David Gallo; John Brumfield; Leo E Otterbein; Brian S Zuckerbraun
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Authors:  Inge Bauer; Benedikt H J Pannen
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