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缺氧对肺基因表达和蛋白质组学特征的影响:对肺表面活性物质反应的见解。

Effect of hypoxia on lung gene expression and proteomic profile: insights into the pulmonary surfactant response.

作者信息

Olmeda Bárbara, Umstead Todd M, Silveyra Patricia, Pascual Alberto, López-Barneo José, Phelps David S, Floros Joanna, Pérez-Gil Jesús

机构信息

Dept. Bioquímica, Fac. Biología, Universidad Complutense, Madrid, Spain.

Center for Host Defense, Inflammation, and Lung Disease (CHILD), Department of Pediatrics, The Pennsylvania State University College of Medicine, Hershey, PA, USA.

出版信息

J Proteomics. 2014 Apr 14;101:179-91. doi: 10.1016/j.jprot.2014.02.019. Epub 2014 Feb 24.

Abstract

UNLABELLED

Exposure of lung to hypoxia has been previously reported to be associated with significant alterations in the protein content of bronchoalveolar lavage (BAL) and lung tissue. In the present work we have used a proteomic approach to describe the changes in protein complement induced by moderate long-term hypoxia (rats exposed to 10% O2 for 72h) in BAL and lung tissue, with a special focus on the proteins associated with pulmonary surfactant, which could indicate adaptation of this system to limited oxygen availability. The analysis of the general proteomic profile indicates a hypoxia-induced increase in proteins associated with inflammation both in lavage and lung tissue. Analysis at mRNA and protein levels revealed no significant changes induced by hypoxia on the content in surfactant proteins or their apparent oligomeric state. In contrast, we detected a hypoxia-induced significant increase in the expression and accumulation of hemoglobin in lung tissue, at both mRNA and protein levels, as well as an accumulation of hemoglobin both in BAL and associated with surface-active membranes of the pulmonary surfactant complex. Evaluation of pulmonary surfactant surface activity from hypoxic rats showed no alterations in its spreading ability, ruling out inhibition by increased levels of serum or inflammatory proteins.

BIOLOGICAL SIGNIFICANCE

This work reveals that hypoxia induces extensive changes in the proteomic profile of lung bronchoalveolar lavage, including the presence of proteins related with inflammation both in lung tissue and lavage, and a significant increase in the synthesis and secretion by the lung tissue of different forms of hemoglobin. The level of specific pulmonary surfactant-associated proteins is not substantially altered due to hypoxia, but hypoxia-adapted surfactant exhibits an enhanced ability to form surface-active films at the air-liquid interface. The increased amount of β-globin integrated into the operative surfactant complexes obtained from hypoxic rats is a relevant feature that points to the existence of adaptive responses coupling surfactant function and oxygen availability.

摘要

未标记

先前有报道称,肺暴露于低氧环境与支气管肺泡灌洗(BAL)液和肺组织中的蛋白质含量显著改变有关。在本研究中,我们采用蛋白质组学方法描述中度长期低氧(大鼠暴露于10%氧气72小时)诱导的BAL液和肺组织中蛋白质组成的变化,特别关注与肺表面活性物质相关的蛋白质,这可能表明该系统对有限氧气供应的适应性。对总体蛋白质组图谱的分析表明,低氧诱导灌洗液和肺组织中与炎症相关的蛋白质增加。在mRNA和蛋白质水平的分析显示,低氧对表面活性物质蛋白的含量或其明显的寡聚状态没有显著影响。相反,我们在mRNA和蛋白质水平均检测到低氧诱导肺组织中血红蛋白的表达和积累显著增加,以及BAL液中血红蛋白的积累和与肺表面活性物质复合物表面活性膜相关的血红蛋白积累。对低氧大鼠肺表面活性物质表面活性的评估显示其铺展能力没有改变,排除了血清或炎症蛋白水平升高的抑制作用。

生物学意义

这项研究表明,低氧诱导肺支气管肺泡灌洗蛋白质组图谱发生广泛变化,包括肺组织和灌洗液中与炎症相关蛋白质的存在,以及肺组织合成和分泌不同形式血红蛋白的显著增加。低氧不会使特定的肺表面活性物质相关蛋白水平发生实质性改变,但适应低氧的表面活性物质在气液界面形成表面活性膜的能力增强。整合到低氧大鼠获得的活性表面活性物质复合物中的β-珠蛋白量增加是一个相关特征,表明存在将表面活性物质功能与氧气供应相耦合的适应性反应。

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