Modification of cyclophosphamide-induced pulmonary toxicity in normal mice.

M J Allalunis-Turner, D W Siemann
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Abstract

The effects of fractionated doses, in vivo thiol modulation, and antifibrinolytic therapy on the expression of lung damage induced by cyclophosphamide (Cy) were evaluated in C3H mice. The protein content of lung lavage samples taken 4 days after Cy treatment was used as an early indicator of damage. In fractionation studies, little difference in lung protein was observed when 200 mg of Cy/kg was administered as a single dose or as two or four equal doses given daily, suggesting that little sparing effect occurred with fractionated doses of Cy. In experiments that tested the effects of exogenous thiol administration, mice treated with WR-2721 before Cy were protected against lung damage, whereas the use of sodium thiosulfate or mesna did not give this protection. Treatment with epsilon-aminocaproic acid, which inhibits the breakdown of fibrin clots, did not result in enhanced Cy damage as measured by lung lavage or breathing rate; this suggests that the extended presence of fibrin per se did not contribute to Cy-induced pulmonary damage.

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环磷酰胺致正常小鼠肺毒性的修饰。
在C3H小鼠中,研究了分级剂量、体内硫醇调节和抗纤溶治疗对环磷酰胺(Cy)诱导肺损伤表达的影响。Cy治疗4天后肺灌洗标本的蛋白质含量作为损伤的早期指标。在分离研究中,当200 mg /kg的Cy作为单次剂量或每天给予2次或4次等量剂量时,肺蛋白几乎没有差异,这表明分离剂量的Cy几乎没有保留作用。在测试外源性硫醇给药效果的实验中,在Cy之前用WR-2721治疗的小鼠可以防止肺损伤,而使用硫代硫酸钠或mesna则没有这种保护作用。用抑制纤维蛋白凝块分解的epsilon-氨基己酸治疗,通过肺灌洗或呼吸频率测量,并未导致Cy损伤增强;这表明纤维蛋白本身的延长存在并不会导致cy诱导的肺损伤。
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