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肝脏分泌的荧光血 plasma 标志物可实现对微循环的慢性成像。

Liver-secreted fluorescent blood plasma markers enable chronic imaging of the microcirculation.

机构信息

Center for Translational Neuromedicine, Faculty of Health and Life Sciences, University of Copenhagen, Copenhagen, Denmark.

Viral Vector Core, Gunma University Initiative for Advanced Research, Maebashi, Gunma 371-8511, Japan.

出版信息

Cell Rep Methods. 2022 Sep 21;2(10):100302. doi: 10.1016/j.crmeth.2022.100302. eCollection 2022 Oct 24.

Abstract

Studying blood microcirculation is vital for gaining insights into vascular diseases. Blood flow imaging in deep tissue is currently achieved by acute administration of fluorescent dyes in the blood plasma. This is an invasive process, and the plasma fluorescence decreases within an hour of administration. Here, we report an approach for the longitudinal study of vasculature. Using a single intraperitoneal or intravenous administration of viral vectors, we express fluorescent secretory albumin-fusion proteins in the liver to chronically label the blood circulation in mice. This approach allows for longitudinal observation of circulation from 2 weeks to over 4 months after vector administration. We demonstrate the chronic assessment of vascular functions including functional hyperemia and vascular plasticity in micro- and mesoscopic scales. This genetic plasma labeling approach represents a versatile and cost-effective method for the chronic investigation of vasculature functions across the body in health and disease animal models.

摘要

研究血液微循环对于深入了解血管疾病至关重要。目前,通过在血液血浆中急性给药荧光染料来实现深层组织中的血流成像。这是一种侵入性过程,给药后一小时内血浆荧光会减弱。在这里,我们报告了一种用于血管系统纵向研究的方法。通过单次腹腔内或静脉内给予病毒载体,我们在肝脏中表达荧光分泌型白蛋白融合蛋白,以在小鼠中长期标记血液循环。这种方法允许在载体给药后 2 周到 4 个月以上的时间内进行循环的纵向观察。我们展示了在微观和介观尺度上对包括功能性充血和血管可塑性在内的血管功能进行慢性评估。这种遗传血浆标记方法代表了一种通用且具有成本效益的方法,可用于在健康和疾病动物模型中对全身血管功能进行慢性研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2f13/9606131/10a412419218/fx1.jpg

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