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健康人体呼吸道细菌种群的地域连续性。

Topographical continuity of bacterial populations in the healthy human respiratory tract.

机构信息

University of Pennsylvania School of Medicine, 3610 Hamilton Walk, Philadelphia, PA 19104, USA.

出版信息

Am J Respir Crit Care Med. 2011 Oct 15;184(8):957-63. doi: 10.1164/rccm.201104-0655OC. Epub 2011 Jun 16.

Abstract

RATIONALE

Defining the biogeography of bacterial populations in human body habitats is a high priority for understanding microbial-host relationships in health and disease. The healthy lung was traditionally considered sterile, but this notion has been challenged by emerging molecular approaches that enable comprehensive examination of microbial communities. However, studies of the lung are challenging due to difficulties in working with low biomass samples.

OBJECTIVES

Our goal was to use molecular methods to define the bacterial microbiota present in the lungs of healthy individuals and assess its relationship to upper airway populations.

METHODS

We sampled respiratory flora intensively at multiple sites in six healthy individuals. The upper tract was sampled by oral wash and oro-/nasopharyngeal swabs. Two bronchoscopes were used to collect samples up to the glottis, followed by serial bronchoalveolar lavage and lower airway protected brush. Bacterial abundance and composition were analyzed by 16S rDNA Q-PCR and deep sequencing.

MEASUREMENTS AND MAIN RESULTS

Bacterial communities from the lung displayed composition indistinguishable from the upper airways, but were 2 to 4 logs lower in biomass. Lung-specific sequences were rare and not shared among individuals. There was no unique lung microbiome.

CONCLUSIONS

In contrast to other organ systems, the respiratory tract harbors a homogenous microbiota that decreases in biomass from upper to lower tract. The healthy lung does not contain a consistent distinct microbiome, but instead contains low levels of bacterial sequences largely indistinguishable from upper respiratory flora. These findings establish baseline data for healthy subjects and sampling approaches for sequence-based analysis of diseases.

摘要

背景

定义人体栖息地中细菌种群的生物地理学是理解健康和疾病中微生物-宿主关系的当务之急。健康的肺传统上被认为是无菌的,但新兴的分子方法使人们能够全面检查微生物群落,这一观点受到了挑战。然而,由于处理低生物量样本的困难,对肺部的研究具有挑战性。

目的

我们的目标是使用分子方法定义健康个体肺部存在的细菌微生物群,并评估其与上呼吸道群体的关系。

方法

我们在六名健康个体的多个部位密集采样呼吸菌群。上呼吸道通过口腔冲洗和口咽/鼻咽拭子采样。使用两个支气管镜收集直至声门的样本,然后进行连续支气管肺泡灌洗和下呼吸道保护刷。通过 16S rDNA Q-PCR 和深度测序分析细菌丰度和组成。

测量和主要结果

来自肺部的细菌群落与上呼吸道的组成无法区分,但生物量低 2 到 4 个对数级。肺部特异性序列很少,个体之间不共享。没有独特的肺部微生物组。

结论

与其他器官系统相比,呼吸道具有同质的微生物群,从上部到下部的生物量减少。健康的肺不包含一致的独特微生物组,而是包含大量与上呼吸道菌群难以区分的低水平细菌序列。这些发现为健康受试者建立了基线数据,并为基于序列的疾病分析提供了采样方法。

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Topographical continuity of bacterial populations in the healthy human respiratory tract.健康人体呼吸道细菌种群的地域连续性。
Am J Respir Crit Care Med. 2011 Oct 15;184(8):957-63. doi: 10.1164/rccm.201104-0655OC. Epub 2011 Jun 16.

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