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2
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本文引用的文献

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The level and half-life of glutathione in human plasma.人体血浆中谷胱甘肽的水平及半衰期。
FEBS Lett. 1980 Nov 3;120(2):209-11. doi: 10.1016/0014-5793(80)80299-7.
2
Tumor cell anti-oxidant defenses. Inhibition of the glutathione redox cycle enhances macrophage-mediated cytolysis.肿瘤细胞的抗氧化防御。谷胱甘肽氧化还原循环的抑制增强巨噬细胞介导的细胞溶解作用。
J Exp Med. 1981 Apr 1;153(4):766-82. doi: 10.1084/jem.153.4.766.
3
Mechanism of augmentation of the antibody response in vitro by 2-mercaptoethanol in murine lymphocytes. I. 2-Mercaptoethanol-induced stimulation of the uptake of cystine, an essential amino acid.2-巯基乙醇对小鼠淋巴细胞体外抗体应答增强作用的机制。I. 2-巯基乙醇诱导对必需氨基酸胱氨酸摄取的刺激作用。
J Exp Med. 1982 May 1;155(5):1277-90. doi: 10.1084/jem.155.5.1277.
4
Inhibition of lectin-induced lymphocyte activation by 2-cyclohexene-1-one: decreased intracellular glutathione inhibits an early event in the activation sequence.2-环己烯-1-酮对凝集素诱导的淋巴细胞活化的抑制作用:细胞内谷胱甘肽减少会抑制活化序列中的早期事件。
J Immunol. 1981 Dec;127(6):2257-62.
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Selective modification of glutathione metabolism.谷胱甘肽代谢的选择性修饰。
Science. 1983 Apr 29;220(4596):472-7. doi: 10.1126/science.6836290.
6
Glutathione depletion sensitizes tumor cells to oxidative cytolysis.谷胱甘肽耗竭使肿瘤细胞对氧化性细胞溶解敏感。
J Biol Chem. 1982 Feb 10;257(3):1231-7.
7
Glutathione disulfide (GSSG) efflux from cells and tissues.谷胱甘肽二硫化物(GSSG)从细胞和组织中的流出。
Methods Enzymol. 1984;105:445-51. doi: 10.1016/s0076-6879(84)05062-x.
8
Glutathione redox cycle protects cultured endothelial cells against lysis by extracellularly generated hydrogen peroxide.谷胱甘肽氧化还原循环可保护培养的内皮细胞免受细胞外产生的过氧化氢的裂解作用。
J Clin Invest. 1984 Mar;73(3):706-13. doi: 10.1172/JCI111263.
9
Plasma glutathione and glutathione disulfide in the rat: regulation and response to oxidative stress.大鼠血浆中的谷胱甘肽和二硫化谷胱甘肽:调节及对氧化应激的反应
J Pharmacol Exp Ther. 1983 Dec;227(3):749-54.
10
Pathogenesis of the adult respiratory distress syndrome. Evidence of oxidant activity in bronchoalveolar lavage fluid.成人呼吸窘迫综合征的发病机制。支气管肺泡灌洗液中氧化活性的证据。
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通过直接给予谷胱甘肽气雾剂增加下呼吸道上皮衬液中的谷胱甘肽。

Augmentation of glutathione in the fluid lining the epithelium of the lower respiratory tract by directly administering glutathione aerosol.

作者信息

Buhl R, Vogelmeier C, Critenden M, Hubbard R C, Hoyt R F, Wilson E M, Cantin A M, 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

Proc Natl Acad Sci U S A. 1990 Jun;87(11):4063-7. doi: 10.1073/pnas.87.11.4063.

DOI:10.1073/pnas.87.11.4063
PMID:2349219
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC54047/
Abstract

Glutathione (GSH), a cysteine-containing tripeptide, functions as an antioxidant, provides cells with cysteine, and is required for optimal function of the immune system. Because the epithelial-lining fluid (ELF) of the lower respiratory tract normally contains high GSH levels and lung ELF GSH deficiency states can exist, we evaluated the feasibility of augmenting lung ELF GSH levels by (i) administering GSH to sheep i.v. and by direct aerosolization and then (ii) measuring the GSH levels in lung ELF, lung lymph, venous plasma, and urine. When GSH (600 mg) was administered i.v. (n = 11), GSH levels in venous plasma, lung lymph, and ELF rose, but only transiently, suggesting the i.v. route would not deliver adequate GSH to the alveolar epithelial surface. For directly administering GSH to the lung by the aerosol route, in vitro studies were first conducted to show that greater than 50% of a GSH solution could be converted to droplets less than 3 microns in aerodynamic diameter without oxidizing the GSH. To target functional GSH to the lower respiratory tract, an aerosolized solution of GSH (600 mg) was administered to sheep (n = 12). Significantly, the GSH level in ELF increased 7-fold at 30 min (preaerosol, 45.7 +/- 10 microM; 30-min postaerosol, 337 +/- 64 microM; P less than 0.001). The ELF GSH levels remained above baseline at 1 hr (P less than 0.01), returning toward baseline over a 2-hr period. In contrast, GSH levels in lung lymph, venous plasma, and urine were not significantly increased during the period--i.e., aerosol therapy selectively augmented the GSH levels only at the lung epithelial surface. Thus, functional GSH can be delivered by aerosol to directly augment the ELF GSH levels of the lower respiratory tract. Such an approach may prove useful in treating a variety of lung disorders.

摘要

谷胱甘肽(GSH)是一种含半胱氨酸的三肽,具有抗氧化功能,为细胞提供半胱氨酸,是免疫系统最佳功能所必需的。由于下呼吸道的上皮衬液(ELF)通常含有高浓度的GSH,且可能存在肺ELF GSH缺乏状态,我们评估了通过以下方式提高肺ELF GSH水平的可行性:(i)静脉内给绵羊注射GSH并直接雾化,然后(ii)测量肺ELF、肺淋巴、静脉血浆和尿液中的GSH水平。当静脉内注射GSH(600毫克)时(n = 11),静脉血浆、肺淋巴和ELF中的GSH水平升高,但只是短暂升高,这表明静脉内途径无法将足够的GSH输送到肺泡上皮表面。为了通过雾化途径将GSH直接输送到肺部,首先进行了体外研究,以表明超过50%的GSH溶液可以转化为空气动力学直径小于3微米的液滴,而不会氧化GSH。为了将功能性GSH靶向输送到下呼吸道,给绵羊(n = 12)雾化吸入GSH(600毫克)溶液。值得注意的是,30分钟时ELF中的GSH水平增加了7倍(雾化前,45.7±10微摩尔;雾化后30分钟,337±64微摩尔;P<0.001)。1小时时ELF GSH水平仍高于基线(P<0.01),并在2小时内恢复到基线水平。相比之下,在此期间肺淋巴、静脉血浆和尿液中的GSH水平没有显著增加,即雾化治疗仅选择性地提高了肺上皮表面的GSH水平。因此,功能性GSH可以通过雾化给药直接提高下呼吸道的ELF GSH水平。这种方法可能对治疗多种肺部疾病有用。