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Reversal
of the effect of albumin on gut barrier function in burn by the inhibition of
inducible isoform of nitric oxide synthase.
Chen LW, Wang JS, Hwang B,
Chen JS, Hsu CM.
Arch Surg. 2003
Nov;138(11):1219-25.
Departments
of Surgery and Pathology, Kaohsiung
Veterans
General
Hospital,
National
Yang-Ming
University,
Taipei,
Taiwan.
HYPOTHESIS:
The use of albumin in the early resuscitation formula after major burn has been
forbidden because of its damaging effect on the gut barrier function. We
hypothesize that inhibition of the inducible isoform of nitric oxide synthase to
stabilize endothelial permeability and to retain albumin in the vascular space
will ameliorate the major trauma-induced gut barrier dysfunction.Design,
Interventions, and MAIN OUTCOME MEASURES: In experiment 1, specific
pathogen-free rats undergoing 35% total body surface area burn or sham burn were
given equal volumes (7.5 mL/kg) of isotonic sodium chloride solution or albumin
from femoral veins for fluid resuscitation at 0, 4, or 8 hours after burn. In
experiment 2, intraperitoneal S-methylisothiourea sulfate (7.5 mg/kg) was given
immediately after burn to rats from different groups, as in experiment 1 (SMT
groups). At 24 hours after burn, the intestinal mucosa was assayed for
myeloperoxidase activity as an index for neutrophil sequestration, the
distribution of fluorescein isothiocyanate-dextran across the lumen of small
intestine was determined to evaluate the intestinal permeability, and bacterial
translocation (BT) to the mesenteric lymph nodes (MLNs) and histological
findings in the ileum were also examined. RESULTS: Compared with sham burn, burn
induced significant increases in intestinal mucosa myeloperoxidase activity,
intestinal permeability, BT to the MLNs, and villi sloughing in rats. Albumin
administration at 0 or 4 hours after burn enhanced the increases in neutrophil
sequestration, permeability, and villi sloughing compared with saline injection
at the same times. In contrast, injection of albumin in the burn-SMT group did
not aggravate these changes in intestinal myeloperoxidase activity, intestinal
permeability, BT to the MLNs, and villi edema. Burn-SMT rats with albumin
injections at 4 or 8 hours after burn showed significant 35% and 52% decreases,
respectively, in intestinal permeability compared with burn-SMT-saline rats. Use
of albumin at 8 hours after burn in combination with S-methylisothiourea
significantly attenuated BT to the MLNs and reduced villi edema. CONCLUSIONS:
Early albumin resuscitation aggravated the burn-induced gut damage. Albumin
administration and inhibition of the inducible isoform of nitric oxide synthase
in combination decreased burn-induced gut barrier dysfunction and reversed the
damaging effect of albumin on gut barrier function and decreased
BT.
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