甘露糖结合凝集素在香烟烟雾诱导的肺部炎症中的治疗作用?来自小鼠模型的证据。
Therapeutic role for mannose-binding lectin in cigarette smoke-induced lung inflammation? Evidence from a murine model.
机构信息
Department of Thoracic Medicine, Royal Adelaide Hospital and Lung Research Laboratory, Hanson Institute, Adelaide, South Australia, Australia.
出版信息
Am J Respir Cell Mol Biol. 2010 Feb;42(2):235-42. doi: 10.1165/rcmb.2008-0486OC. Epub 2009 May 1.
Defective efferocytosis in the airway may perpetuate inflammation in smokers with/without chronic obstructive pulmonary disease. Mannose-binding lectin (MBL) improves efferocytosis in vitro; however, the effects of in vivo administration are unknown. MBL circulates in complex with MBL-associated serine proteases (MASPs), and efferocytosis involves activation of cytoskeletal-remodeling molecules, including Rac1/2/3. We hypothesized that MBL would improve efferocytosis in vivo, and that possible mechanisms for this effect would include up-regulation of Rac1/2/3 or MASPs. We used a smoking mouse model to investigate the effects of MBL on efferocytosis. MBL (20 microg/20 g mouse) was administered via nebulizer to smoke-exposed mice. In lung tissue (disaggregated) and bronchoalveolar lavage (BAL), we investigated leukocyte counts, apoptosis, and the ability of alveolar and tissue macrophages to phagocytose apoptotic murine epithelial cells. In human studies, flow cytometry, ELISA, and RT-PCR were used to investigate the effects of MBL on efferocytosis, Rac1/2/3, and MASPs. Smoke-exposed mice showed significantly reduced efferocytosis in BAL and tissue. Efferocytosis was significantly improved by MBL (BAL: control, 26.2%; smoke-exposed, 17.66%; MBL + smoke-exposed, 27.8%; tissue: control, 35.9%; smoke-exposed, 21.6%; MBL + smoke-exposed, 34.5%). Leukocyte/macrophage counts were normalized in smoke-exposed mice treated with MBL. In human studies, MBL was reduced in chronic obstructive pulmonary disease and in smokers, and was significantly correlated with reduced efferocytosis ex vivo. MASPs were not detected in BAL, and were not produced by alveolar or tissue macrophages. MBL significantly increased macrophage expression of Rac1/2/3. We provide evidence for Rac1/2/3 involvement in the MBL-mediated improvement in efferocytosis, and a rationale for investigating MBL as a supplement to existing therapies in smoking-related lung inflammation.
气道中吞噬作用的缺陷可能会使有/无慢性阻塞性肺疾病的吸烟者的炎症持续存在。甘露糖结合凝集素(MBL)可改善体外吞噬作用;然而,其体内给药的效果尚不清楚。MBL 与 MBL 相关丝氨酸蛋白酶(MASP)形成复合物,吞噬作用涉及细胞骨架重塑分子(包括 Rac1/2/3)的激活。我们假设 MBL 将改善体内吞噬作用,其可能的作用机制包括 Rac1/2/3 或 MASPs 的上调。我们使用吸烟小鼠模型来研究 MBL 对吞噬作用的影响。MBL(20μg/20g 小鼠)通过雾化器给予吸烟暴露的小鼠。在肺组织(分散)和支气管肺泡灌洗(BAL)中,我们研究了白细胞计数、凋亡以及肺泡和组织巨噬细胞吞噬凋亡的小鼠上皮细胞的能力。在人体研究中,使用流式细胞术、ELISA 和 RT-PCR 来研究 MBL 对吞噬作用、Rac1/2/3 和 MASPs 的影响。暴露于烟雾的小鼠在 BAL 和组织中的吞噬作用明显降低。MBL 显著改善了吞噬作用(BAL:对照,26.2%;暴露于烟雾,17.66%;MBL+暴露于烟雾,27.8%;组织:对照,35.9%;暴露于烟雾,21.6%;MBL+暴露于烟雾,34.5%)。用 MBL 治疗暴露于烟雾的小鼠后,白细胞/巨噬细胞计数恢复正常。在人体研究中,MBL 在慢性阻塞性肺疾病和吸烟者中减少,并且与体外吞噬作用降低显著相关。BAL 中未检测到 MASPs,肺泡和组织巨噬细胞也未产生。MBL 显著增加了巨噬细胞 Rac1/2/3 的表达。我们提供了 Rac1/2/3 参与 MBL 介导的吞噬作用改善的证据,并为研究 MBL 作为吸烟相关肺炎症现有治疗方法的补充提供了依据。
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