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超氧化物歧化酶的雾化。通过重组人Cu++/Zn++超氧化物歧化酶的雾化增强呼吸道上皮衬液抗氧化屏障。

Aerosolization of superoxide dismutase. Augmentation of respiratory epithelial lining fluid antioxidant screen by aerosolization of recombinant human Cu++/Zn++ superoxide dismutase.

作者信息

Gillissen A, Roum J H, Hoyt R F, Crystal R G

机构信息

Pulmonary Branch, National Heart, Lung, and Blood Institute, National Institutes of Health, Bethesda, MD 20892.

出版信息

Chest. 1993 Sep;104(3):811-5. doi: 10.1378/chest.104.3.811.

DOI:10.1378/chest.104.3.811
PMID:8396002
Abstract

Various human pulmonary diseases are characterized by an increased oxidant burden on the respiratory epithelial surface. As a step toward developing a therapy to augment the antioxidant defenses of respiratory epithelial lining fluid (ELF) of the human lung, we have evaluated the feasibility of aerosolizing a human protein antioxidant to the respiratory epithelial surface of an experimental animal sufficiently large to permit repetitive sampling of ELF. To accomplish this, recombinant human Cu++/Zn++ superoxide dismutase (rSOD) was aerosolized to sheep, and the levels of human superoxide dismutase (SOD) and antisuperoxide anion (O2.-) capacity were quantified in ELF over time. In vitro aerosolization did not alter the specific activity of rSOD (p > 0.5). In vivo aerosolization of rSOD (100 mg) to sheep (n = 7) resulted in peak amounts of human Cu++/Zn++ SOD in ELF of 3.1 +/- 0.6 mumol/L, with a parallel increase in the anti-O2.- capacity of ELF. For the duration of the study (5 h), levels of SOD and anti-O2.- in ELF remained elevated, with a value 50 percent of the peak at 5 h. Aerosolization of phosphate-buffered saline (n = 5) had no effect on SOD or anti-O2.- levels in ELF. In animals receiving rSOD, there was no change in the specific activity of SOD recovered in ELF compared to the starting material (p > 0.4). We conclude that rSOD can be delivered by aerosol to the ELF of a large animal with preservation of specific activity and that a substantial increase in both the amount of SOD and the anti-O2.- capacity can be achieved for a period of time applicable to human therapy, supporting the rationale for evaluation of rSOD aerosol as an antioxidant in human pulmonary disease.

摘要

多种人类肺部疾病的特征是呼吸道上皮表面的氧化应激负担增加。作为开发一种增强人肺呼吸道上皮衬液(ELF)抗氧化防御能力疗法的第一步,我们评估了将一种人类蛋白质抗氧化剂雾化到实验动物呼吸道上皮表面的可行性,该动物体型足够大,以便能够重复采集ELF样本。为实现这一目标,将重组人铜/锌超氧化物歧化酶(rSOD)雾化到绵羊体内,并随时间对ELF中的人超氧化物歧化酶(SOD)水平和抗超氧阴离子(O2.-)能力进行定量分析。体外雾化不会改变rSOD的比活性(p>0.5)。对7只绵羊进行rSOD(100mg)体内雾化后,ELF中人类铜/锌超氧化物歧化酶的峰值量为3.1±0.6μmol/L,同时ELF的抗O2.-能力也相应增加。在研究期间(5小时),ELF中的SOD和抗O2.-水平一直保持升高,5小时时的值为峰值的50%。雾化磷酸缓冲盐水(n = 5)对ELF中的SOD或抗O2.-水平没有影响。在接受rSOD的动物中,与起始材料相比,ELF中回收的SOD比活性没有变化(p>0.4)。我们得出结论,rSOD可以通过雾化方式递送至大型动物的ELF中,且比活性得以保留,并且在适用于人类治疗的时间段内,SOD的量和抗O2.-能力都能显著增加,这为评估rSOD雾化剂作为人类肺部疾病的抗氧化剂提供了理论依据。

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