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基于设计的体视学方法定位人肺中的巨噬细胞。

Localization of Macrophages in the Human Lung via Design-based Stereology.

机构信息

Division of Pulmonary, Critical Care, and Sleep Medicine, Department of Medicine, and.

Division of Pulmonary Sciences and Critical Care Medicine.

出版信息

Am J Respir Crit Care Med. 2020 May 15;201(10):1209-1217. doi: 10.1164/rccm.201911-2105OC.

DOI:10.1164/rccm.201911-2105OC
PMID:32197050
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7233346/
Abstract

Interstitial macrophages (IMs) and airspace macrophages (AMs) play critical roles in lung homeostasis and host defense, and are central to the pathogenesis of a number of lung diseases. However, the absolute numbers of macrophages and the precise anatomic locations they occupy in the healthy human lung have not been quantified. To determine the precise number and anatomic location of human pulmonary macrophages in nondiseased lungs and to quantify how this is altered in chronic cigarette smokers. Whole right upper lobes from 12 human donors without pulmonary disease (6 smokers and 6 nonsmokers) were evaluated using design-based stereology. CD206 (cluster of differentiation 206)-positive/CD43 AMs and CD206/CD43 IMs were counted in five distinct anatomical locations using the optical disector probe. An average of 2.1 × 10 IMs and 1.4 × 10 AMs were estimated per right upper lobe. Of the AMs, 95% were contained in diffusing airspaces and 5% in airways. Of the IMs, 78% were located within the alveolar septa, 14% around small vessels, and 7% around the airways. The local density of IMs was greater in the alveolar septa than in the connective tissue surrounding the airways or vessels. The total number and density of IMs was 36% to 56% greater in the lungs of cigarette smokers versus nonsmokers. The precise locations occupied by pulmonary macrophages were defined in nondiseased human lungs from smokers and nonsmokers. IM density was greatest in the alveolar septa. Lungs from chronic smokers had increased IM numbers and overall density, supporting a role for IMs in smoking-related disease.

摘要

间质巨噬细胞 (IMs) 和肺泡巨噬细胞 (AMs) 在肺稳态和宿主防御中发挥着关键作用,是许多肺部疾病发病机制的核心。然而,巨噬细胞的绝对数量以及它们在健康人肺中的精确解剖位置尚未被量化。为了确定非病变肺中人类肺巨噬细胞的确切数量和解剖位置,并量化其在慢性吸烟人群中的变化。使用基于设计的体视学评估了 12 名无肺部疾病的人类供体的整个右上肺叶(6 名吸烟者和 6 名非吸烟者)。使用光学分割探针在五个不同的解剖位置对 CD206(分化群 206)阳性/CD43 AMs 和 CD206/CD43 IMs 进行计数。估计每个右上肺叶平均有 2.1×10 个 IM 和 1.4×10 个 AM。在 AM 中,95%存在于弥散性气腔中,5%存在于气道中。在 IM 中,78%位于肺泡隔内,14%位于小血管周围,7%位于气道周围。IM 的局部密度在肺泡隔中大于气道或血管周围的结缔组织。与非吸烟者相比,吸烟者肺中的 IM 总数和密度增加了 36%至 56%。在吸烟者和非吸烟者的非病变肺中定义了肺巨噬细胞的精确位置。IM 密度在肺泡隔中最大。慢性吸烟者的 IM 数量和总体密度增加,支持 IM 在与吸烟相关的疾病中发挥作用。

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