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高分辨率活体成像技术在研究小鼠肾脏损伤和感染免疫反应中的应用

High Resolution Intravital Imaging of the Renal Immune Response to Injury and Infection in Mice.

机构信息

Department of Medical Cell Biology, Uppsala University, Uppsala, Sweden.

Swedish Medical Nanoscience Center, Department of Neuroscience, Karolinska Institutet, Stockholm, Sweden.

出版信息

Front Immunol. 2019 Nov 29;10:2744. doi: 10.3389/fimmu.2019.02744. eCollection 2019.

Abstract

We developed an experimental set up that enables longitudinal studies of immune cell behavior in the challenged as well as unchallenged kidney of anesthetized mice over several hours. Using highly controlled vacuum to stabilize the kidney, the superficial renal cortex could continuously be visualized with minimal disruption of the local microenvironment. No visible changes in blood flow or neutrophils and macrophages numbers were observed after several hours of visualizing the unchallenged kidney, indicating a stable tissue preparation without apparent tissue damage. Applying this set up to monocyte/macrophage (CXCR1) reporter mice, we observed the extensive network of stellate-shaped CXCR1 positive cells (previously identified as renal mononuclear phagocytes). The extended dendrites of the CXCR1 positive cells were found to bridge multiple capillaries and tubules and were constantly moving. Light induced sterile tissue injury resulted in rapid neutrophil accumulation to the site of injury. Similarly, microinfusion of uropathogenic into a single nephron induced a rapid and massive recruitment of neutrophils to the site of infection, in addition to active bacterial clearance by neutrophils. In contrast, the kidney resident mononuclear phagocytes were observed to not increase in numbers or migrate toward the site of injury or infection. In conclusion, this model allows for longitudinal imaging of responses to localized kidney challenges in the mouse.

摘要

我们开发了一种实验装置,使我们能够在麻醉小鼠的挑战和未挑战肾脏中进行数小时的免疫细胞行为的纵向研究。使用高度受控的真空来稳定肾脏,可在最小干扰局部微环境的情况下连续可视化浅表肾皮质。在可视化未挑战肾脏数小时后,观察到血流或中性粒细胞和巨噬细胞数量没有明显变化,表明组织准备稳定,没有明显的组织损伤。将该装置应用于单核细胞/巨噬细胞(CXCR1)报告小鼠,我们观察到广泛的星状 CXCR1 阳性细胞(先前被鉴定为肾单核吞噬细胞)网络。发现 CXCR1 阳性细胞的延伸树突跨越多个毛细血管和小管,并不断移动。光诱导的无菌组织损伤导致中性粒细胞迅速积聚到损伤部位。同样,将尿路致病性细菌微注入单个肾单位会导致大量中性粒细胞迅速募集到感染部位,此外,中性粒细胞还能主动清除细菌。相比之下,观察到肾脏固有单核吞噬细胞的数量没有增加,也没有向损伤或感染部位迁移。总之,该模型允许在小鼠中对局部肾脏挑战的反应进行纵向成像。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/79f0/6916672/8caf7f6047ef/fimmu-10-02744-g0001.jpg

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