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慢性肺病小鼠模型中肺动脉微血管树的微计算机断层扫描可视化与定量分析

Microcomputed tomography visualization and quantitation of the pulmonary arterial microvascular tree in mouse models of chronic lung disease.

作者信息

Schneider Ben, Kopf Katrina W, Mason Emma, Dawson Maggie, Coronado Escobar David, Majka Susan M

机构信息

Department of Medicine, Division of Pulmonary, Critical Care & Sleep Medicine National Jewish Health Denver Colorado USA.

Biological Resource Center National Jewish Health Denver Colorado USA.

出版信息

Pulm Circ. 2023 Aug 27;13(3):e12279. doi: 10.1002/pul2.12279. eCollection 2023 Jul.

Abstract

Pulmonary vascular dysfunction is characterized by remodeling and loss of microvessels in the lung and is a major manifestation of chronic lung diseases (CLD). In murine models of CLD, the small arterioles and capillaries are the first and most prevalent vessels that are affected by pruning and remodeling. Thus, visualization of the pulmonary arterial vasculature in three dimensions is essential to define pruning and remodeling both temporally and spatially and its role in the pathogenesis of CLD, aging, and tissue repair. To this end, we have developed a novel method to visualize and quantitate the murine pulmonary arterial circulation using microcomputed tomography (µCT) imaging. Using this perfusion technique, we can quantitate microvessels to approximately 6 µM in diameter. We hypothesize that bleomycin-induced injury would have a significant impact on the arterial vascular structure. As proof of principle, we demonstrated that as a result of bleomycin-induced injury at peak fibrosis, significant alterations in arterial vessel structure were visible in the three-dimensional models as well as quantification. Thus, we have successfully developed a perfusion methodology and complementary analysis techniques, which allows for the reconstruction, visualization, and quantitation of the mouse pulmonary arterial microvasculature in three-dimensions. This tool will further support the examination and understanding of angiogenesis during the development of CLD as well as repair following injury.

摘要

肺血管功能障碍的特征是肺微血管重塑和丢失,是慢性肺部疾病(CLD)的主要表现。在CLD的小鼠模型中,小动脉和毛细血管是最早且最普遍受到修剪和重塑影响的血管。因此,三维可视化肺动脉血管系统对于在时间和空间上定义修剪和重塑及其在CLD、衰老和组织修复发病机制中的作用至关重要。为此,我们开发了一种使用微型计算机断层扫描(µCT)成像来可视化和定量小鼠肺动脉循环的新方法。使用这种灌注技术,我们可以定量直径约为6微米的微血管。我们假设博来霉素诱导的损伤会对动脉血管结构产生重大影响。作为原理证明,我们证明在纤维化高峰期,由于博来霉素诱导的损伤,三维模型以及定量分析中均可见动脉血管结构的显著改变。因此,我们成功开发了一种灌注方法和互补分析技术,能够在三维空间中重建、可视化和定量小鼠肺动脉微血管系统。该工具将进一步支持对CLD发展过程中的血管生成以及损伤后修复的检查和理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5a79/10461042/32e79ad83ed5/PUL2-13-e12279-g003.jpg

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