Literature DB >> 2384071

Evaluation of N-acetylcysteine and methylprednisolone as therapies for oxygen and acrolein-induced lung damage.

J A Critchley1, J M Beeley, R J Clark, M Summerfield, S Bell, M S Spurlock, J A Edginton, J D Buchanan.   

Abstract

Reactive oxidizing species are implicated in the etiology of a range of inhalational pulmonary injuries. Consequently, various free radical scavengers have been tested as potential prophylactic agents. The sulfydryl compound, N-acetylcysteine (NAC) is the only such compound clinically available for use in realistic dosages, and it is well established as an effective antidote for the hepatic and renal toxicity of paracetamol. Another approach in pulmonary injury prophylaxis is methylprednisolone therapy. We evaluated NAC and methylprednisolone in two rat models of inhalational injury: 40-hr exposure to greater than 97% oxygen at 1.1 bar and 15-min exposure to acrolein vapor (210 ppm). For oxygen toxicity, NAC (80 mg) or methylprednisolone (10 mg) were given IP every 2 or 6 hr, respectively. For acrolein, single doses of NAC (1 g/kg) and methylprednisolone (30 mg/kg) were given intravenously 15 min before exposure. In sham-exposed control animals, neither treatment favorably effected mortality, lung wet/dry weight ratios, or pulmonary histology. The increases in lung wet/dry weight ratios, seen with both oxygen and acrolein toxicity were reduced with both treatments. However, with oxygen, NAC therapy was associated with considerably increased mortality and histological changes. Furthermore, IP NAC administration resulted in large volumes of ascitic fluid. With acrolein, IV, NAC had no significant effect on mortality or pulmonary histological damage. Methylprednisolone had no beneficial effects on either the mortality or histological damage observed in either toxicity model. We caution against the ad hoc use of NAC in the management of inhalational pulmonary injury.

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Year:  1990        PMID: 2384071      PMCID: PMC1568328          DOI: 10.1289/ehp.85-1568328

Source DB:  PubMed          Journal:  Environ Health Perspect        ISSN: 0091-6765            Impact factor:   9.031


  19 in total

1.  Effect of various substances on survival times of mice exposed to different high oxygen tensions.

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2.  Oxygen poisoning and x-irradiation: a mechanism in common.

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Review 3.  Oxy-radicals and related species: their formation, lifetimes, and reactions.

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Review 4.  The relation of free radical production to hyperoxia.

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5.  Interaction of N-acetylcysteine and bleomycin on hyperbaric oxygen-induced lung damage in mice.

Authors:  D D Jamieson; D R Kerr; I Unsworth
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Review 6.  Lung protection by thiol-containing antioxidants.

Authors:  I A Cotgreave; P Moldéus
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7.  Effect of oral N-acetylcysteine administration on human blood neutrophil and monocyte function.

Authors:  T Jensen; A Kharazmi; P O Schiøtz; H Nielsen; S Stenvang Pedersen; G Stafanger; C Koch; N Høiby
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8.  The toxicity of N-acetylcysteine in laboratory animals.

Authors:  R E Johnston; H C Hawkins; J H Weikel
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9.  In vivo metabolism of the cardiovascular toxin, allylamine.

Authors:  P J Boor; R Sanduja; T J Nelson; G A Ansari
Journal:  Biochem Pharmacol       Date:  1987-12-15       Impact factor: 5.858

Review 10.  ARDS after accidental inhalation of zinc chloride smoke.

Authors:  E Hjortsø; J Qvist; M I Bud; J L Thomsen; J B Andersen; F Wiberg-Jørgensen; N K Jensen; R Jones; L M Reid; W M Zapol
Journal:  Intensive Care Med       Date:  1988       Impact factor: 17.440

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  2 in total

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2.  Müller glial dysfunction during diabetic retinopathy in rats is reduced by the acrolein-scavenging drug, 2-hydrazino-4,6-dimethylpyrimidine.

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