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隐球菌病小鼠模型中真菌播散到脑部的敏感生物发光成像。

Sensitive bioluminescence imaging of fungal dissemination to the brain in mouse models of cryptococcosis.

机构信息

Biomedical MRI, Department of Imaging and Pathology, KU Leuven, 3000 Leuven, Belgium.

Molecular Small Animal Imaging Center (MoSAIC), KU Leuven, 3000 Leuven, Belgium.

出版信息

Dis Model Mech. 2019 Jun 17;12(6):dmm039123. doi: 10.1242/dmm.039123.

Abstract

is a leading cause of fungal brain infection, but the mechanism of dissemination and dynamics of cerebral infection following pulmonary disease are poorly understood. To address these questions, non-invasive techniques that can study the dynamic processes of disease development and progression in living animal models or patients are required. As such, bioluminescence imaging (BLI) has emerged as a powerful tool to evaluate the spatial and temporal distribution of infection in living animals. We aimed to study the time profile of the dissemination of cryptococcosis from the lung to the brain in murine models by engineering the first bioluminescent KN99α strain, expressing a sequence-optimized red-shifted luciferase. The high pathogen specificity and sensitivity of BLI was complemented by the three-dimensional anatomical information from micro-computed tomography (μCT) of the lung and magnetic resonance imaging (MRI) of the brain. These non-invasive imaging techniques provided longitudinal readouts on the spatial and temporal distribution of infection following intravenous, intranasal or endotracheal routes of inoculation. Furthermore, the imaging results correlated strongly with the fungal load in the respective organs. By obtaining dynamic and quantitative information about the extent and timing of brain infections for individual animals, we found that dissemination to the brain after primary infection of the lung is likely a late-stage event with a timeframe that is variable between animals. This novel tool in research can aid the identification of host and pathogen factors involved in this process, and supports development of novel preventive or therapeutic approaches.

摘要

新型隐球菌是导致真菌性脑部感染的主要原因,但肺部疾病后传播和大脑感染的动态机制仍不清楚。为了解决这些问题,需要能够研究活体动物模型或患者中疾病发展和进展的动态过程的非侵入性技术。因此,生物发光成像 (BLI) 已成为评估活体动物感染的空间和时间分布的有力工具。我们旨在通过工程化第一个表达经序列优化的红移荧光素酶的生物发光 KN99α 菌株,来研究鼠模型中新型隐球菌从肺部向脑部传播的时间进程。BLI 的高病原体特异性和敏感性通过肺部的微计算机断层扫描 (μCT) 和脑部的磁共振成像 (MRI) 的三维解剖学信息得到补充。这些非侵入性成像技术提供了静脉内、鼻内或气管内接种后感染的空间和时间分布的纵向读数。此外,成像结果与相应器官中的真菌负荷密切相关。通过获得个体动物脑部感染的程度和时间的动态和定量信息,我们发现肺部原发性感染后向大脑的传播很可能是一个晚期事件,其时间框架在动物之间是可变的。这种新型研究工具可以帮助确定涉及该过程的宿主和病原体因素,并支持开发新的预防或治疗方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a382/6602310/fb1612173496/dmm-12-039123-g1.jpg

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