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结核分枝杆菌菌株的传播表型在机制上与诱导不同的肺部病理有关。

Transmission phenotype of Mycobacterium tuberculosis strains is mechanistically linked to induction of distinct pulmonary pathology.

机构信息

Rutgers University-New Jersey Medical School, Department of Medicine, Centre for Emerging Pathogens, Newark, New Jersey, United States of America.

Cellular and Molecular Immunology Laboratory, Núcleo de Doenças Infecciosas, Universidade Federal do Espírito Santo, Vitória, Brazil.

出版信息

PLoS Pathog. 2019 Mar 6;15(3):e1007613. doi: 10.1371/journal.ppat.1007613. eCollection 2019 Mar.

Abstract

In a study of household contacts (HHC), households were categorized into High (HT) and Low (LT) transmission groups based on the proportion of HHC with a positive tuberculin skin test. The Mycobacterium tuberculosis (Mtb) strains from HT and LT index cases of the households were designated Mtb-HT and Mtb-LT, respectively. We found that C3HeB/FeJ mice infected with Mtb-LT strains exhibited significantly higher bacterial burden compared to Mtb-HT strains and also developed diffused inflammatory lung pathology. In stark contrast, a significant number of mice infected with Mtb-HT strains developed caseating granulomas, a lesion type with high potential to cavitate. None of the Mtb-HT infected animals developed diffused inflammatory lung pathology. A link was observed between increased in vitro replication of Mtb-LT strains and their ability to induce significantly high lipid droplet formation in macrophages. These results support that distinct early interactions of Mtb-HT and Mtb-LT strains with macrophages and subsequent differential trajectories in pathological disease may be the mechanism underlying their transmission potential.

摘要

在一项家庭接触者(HHC)的研究中,根据 HHC 中结核菌素皮肤试验阳性者的比例,将家庭分为高(HT)和低(LT)传播组。来自 HT 和 LT 家庭索引病例的结核分枝杆菌(Mtb)菌株分别被指定为 Mtb-HT 和 Mtb-LT。我们发现,感染 Mtb-LT 株的 C3HeB/FeJ 小鼠与 Mtb-HT 株相比,细菌负荷明显更高,并且还表现出弥漫性炎症性肺病理学。相比之下,大量感染 Mtb-HT 株的小鼠形成了干酪样肉芽肿,这是一种具有高潜在空洞的病变类型。没有感染 Mtb-HT 的动物出现弥漫性炎症性肺病理学。在体外,Mtb-LT 株的复制增加与它们诱导巨噬细胞中脂质滴形成显著增加之间存在关联。这些结果表明,Mtb-HT 和 Mtb-LT 菌株与巨噬细胞的早期相互作用不同,以及随后在病理疾病中的不同轨迹可能是其传播潜力的机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6e99/6422314/9ffef280278f/ppat.1007613.g001.jpg

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