Influence of acetylsalicylic acid on development of radiation-induced nephropathy

Purpose : Previous studies have demonstrated that long-term treatment with acetylsalicylic acid (ASA) can significantly reduce the renal functional impairment that develops after high doses of irradiation. The effect is hypothesized to be mediated by selective inhibition of thromboxane A 2 synthesis...

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Bibliographic Details
Published in:International journal of radiation biology 2000, Vol.76 (11), p.1565-1573
Main Authors: VAN KLEEF, E. M, TE POELE, J. A. M, OUSSOREN, Y. G, VAN DER WAL, A, DEWIT, L. G. H, STEWART, F. A
Format: Article
Language:English
Subjects:
Animals
Aspirin - pharmacology
Biological and medical sciences
Dose-Response Relationship, Radiation
Edetic Acid
Female
Humans
In Vitro Techniques
Kidney Diseases - pathology
Kidney Diseases - physiopathology
Kidney Diseases - prevention & control
Kidney Function Tests
Kidneys
Medical sciences
Mice
Mice, Inbred C3H
Nephrology. Urinary tract diseases
Platelet Aggregation - drug effects
Radiation Injuries, Experimental - pathology
Radiation Injuries, Experimental - physiopathology
Radiation Injuries, Experimental - prevention & control
Thromboxane A2 - biosynthesis
Time Factors
Urinary system involvement in other diseases. Miscellaneous
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Summary:Purpose : Previous studies have demonstrated that long-term treatment with acetylsalicylic acid (ASA) can significantly reduce the renal functional impairment that develops after high doses of irradiation. The effect is hypothesized to be mediated by selective inhibition of thromboxane A 2 synthesis and inhibition of platelet aggregation. The present study was undertaken to investigate this phenomenon further using more clinically relevant fractionated and re-irradiation schedules. Methods and materials : Groups of mice were given bilateral renal irradiation with a series of four or 20 daily fractions of X-rays, or 10 daily fractions with a single dose of re-irradiation (0-10Gy) after 27 weeks. Half the mice received ASA in drinking water (2.4 g.l -1) from 1 week before the start of irradiation and continuously throughout the follow-up period. Renal function was assessed by clearance of [ 51 Cr]EDTA, about every 4 weeks for up to 80 weeks after the start of treatment. Histological damage in representative groups of mice was also assessed. Results : Oral administration of ASA caused inhibition of thromboxane A2 synthesis (to < 36% of controls) and a strong inhibition of platelet aggregation in whole mouse blood (ex vivo) . Prolonged treatment with ASA also resulted in a small, non-significant reduction of radiation-induced renal functional damage. No reduction in histological damage was seen in the ASA treated mice. Conclusion : Long-term oral administration of ASA gave only a modest, non-significant reduction of renal radiation injury after clinically relevant fractionated irradiation schedules.
ISSN:0955-3002
1362-3095
DOI:10.1080/09553000050176324