IL-1 receptor antagonist as an aerosol in inflammation.

Alexander M Ischenko, Boris P Nikolaev, Tatiana V Kotova, Eugeny V Vorobeychikov, Velentina G Konusova, Ludmila Y Yakovleva
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引用次数: 4

Abstract

The feasibility of efficient aerosol delivery of the human IL-1 receptor antagonist (IL-1Ra) for reduction of acute lung inflammation was demonstrated in a mouse model study. The therapeutic efficacy of dry powder formulations PM(2), PM(10) of IL-1Ra was studied at nonforced inhalation in an aerosol chamber using the DPI "Spinhaler". Micronized powder formulations for insufflation were produced by air-jet milling. The anti-inflammatory effect of IL-Ra preparation was assessed by differential cell counts and biochemical composition of bronchoalveolar lavage (BAL). Reactive oxygen species (ROS), metabolic parameters of BAL (pH, redox potential, total protein, and lactate), and morphological lung changes were investigated by methods of luminol-dependent chemoluminescence, electrochemistry, microscopy, optical, and NMR spectroscopy. Inhalation of IL-1Ra aerosol ensured the systemic absorption of IL-1Ra in the circulatory system and reduced the acute inflammatory response to intranasal lipopolysaccharide challenge. The inhaled anti-inflammatory dosage in aerosol administration appeared to be comparable with i.p. injection. The mechanism of positive action of pulmonary aerosol delivery of Il-Ra includes normalization of the oxidative activity of bronchoalveolar cells, prevention of neutrophil recruitment to the bronchoalveolar tract, and improving of cell respiration. The results were used to develop mathematical models of the anti-inflammatory effects of IL-Ra as functions of the doses and dispersion grades of IL-Ra preparations. Aerosol application of IL-Ra may be an apparent way for prophylactic treating of respiratory inflammation caused by bacterial antigens.

IL-1受体拮抗剂在炎症中的气溶胶作用。
在小鼠模型研究中证明了有效的气溶胶输送人类IL-1受体拮抗剂(IL-1Ra)减少急性肺部炎症的可行性。采用DPI“Spinhaler”在气雾室中非强制吸入,研究了IL-1Ra干粉制剂PM(2)、PM(10)的治疗效果。采用喷气铣削技术制备了用于充气的微粉配方。通过支气管肺泡灌洗(BAL)的细胞计数和生化组成来评价IL-Ra制剂的抗炎作用。通过鲁米诺依赖性化学发光、电化学、显微镜、光学和核磁共振等方法研究活性氧(ROS)、BAL代谢参数(pH、氧化还原电位、总蛋白和乳酸)和肺形态学变化。吸入IL-1Ra气雾剂确保了循环系统对IL-1Ra的全身吸收,并减少了鼻内脂多糖攻击的急性炎症反应。雾化给药的吸入抗炎剂量似乎与滴注相当。肺气溶胶输送Il-Ra的积极作用机制包括支气管肺泡细胞氧化活性正常化,防止中性粒细胞向支气管肺泡道募集,改善细胞呼吸。研究结果建立了IL-Ra抗炎作用随IL-Ra制剂剂量和分散等级变化的数学模型。IL-Ra雾化应用可能是预防性治疗细菌抗原引起的呼吸道炎症的一种明显途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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