Division of Nephrology and Hypertension, Department of Internal Medicine, Inha University School of Medicine, Incheon, South Korea.
Division of Nephrology, Department of Internal Medicine, Kyung Hee University, College of Medicine, Seoul, South Korea.
Front Immunol. 2022 Mar 10;13:844919. doi: 10.3389/fimmu.2022.844919. eCollection 2022.
Traditional histologic methods are limited in detecting dynamic changes in immune cells during acute kidney injury (AKI). Recently, optical tissue clearing combined with multiphoton microscopy (MPM) or light sheet fluorescence microscopy (LSFM) has become an emerging method for deep tissue evaluation and three-dimensional visualization. These new approaches have helped expand our understanding of tissue injury and repair processes, including tracing the changes in immune cells. We designed this study to investigate the morphological and functional alterations of renal mononuclear phagocytes (MNPs) in lipopolysaccharide (LPS)-induced AKI using renal clearing in CD11c-YFP mice. We also evaluated the effect of the NLRP3 inhibitor MCC950 to determine whether NLRP3 inhibition attenuates the activation of CD11c+ cells in an LPS-induced AKI model. Transverse sectioned whole mouse kidney imaging by LSFM showed that CD11c+ cells were mainly distributed in the cortex, especially the tubulointerstitial area. The number of CD11c+ cells was significantly more densely interspersed, particularly in periglomerular and perivascular lesions, in the saline-treated LPS-exposed kidney than in the control kidney. Deep imaging of the kidney cortex by MPM demonstrated an increased number of CD11c+ cells in the saline-treated LPS group compared with the control group. This quantitative alteration of CD11c+ cells in AKI was accompanied by morphological changes at high resolution, showing an increased number and level of dendrites. These morphological and behavioral changes in the saline-treated LPS group were accompanied by increased MHC class II and CD86 on CD11c-YFP+ cells. MCC950 attenuated the activation of CD11c+ cells after AKI and improved renal function. In conclusion, wide and deep three-dimensional visualization using MPM or LSFM combined with kidney clearing uncovers dynamic changes of renal MNPs, which are directly linked to renal function in AKI.
传统的组织学方法在检测急性肾损伤 (AKI) 期间免疫细胞的动态变化方面存在局限性。最近,光学组织透明化结合多光子显微镜 (MPM) 或光片荧光显微镜 (LSFM) 已成为深层组织评估和三维可视化的新兴方法。这些新方法有助于扩展我们对组织损伤和修复过程的理解,包括追踪免疫细胞的变化。我们设计了这项研究,以使用 CD11c-YFP 小鼠的肾脏清除法来研究脂多糖 (LPS) 诱导的 AKI 中肾脏单核吞噬细胞 (MNP) 的形态和功能改变。我们还评估了 NLRP3 抑制剂 MCC950 的作用,以确定 NLRP3 抑制是否能减轻 LPS 诱导的 AKI 模型中 CD11c+细胞的激活。LSFM 对横向切片全鼠肾成像显示,CD11c+细胞主要分布在皮质,特别是肾小管间质区。与对照肾脏相比,在盐水处理的 LPS 暴露肾脏中,CD11c+细胞的数量明显更密集地散布,尤其是在肾小球旁和血管周围病变中。MPM 对肾脏皮质的深层成像显示,与对照组相比,在盐水处理的 LPS 组中 CD11c+细胞的数量增加。AKI 中 CD11c+细胞的这种定量改变伴随着高分辨率下的形态变化,显示出树突数量和水平的增加。盐水处理的 LPS 组中的这些形态和行为变化伴随着 CD11c-YFP+细胞上 MHC 类 II 和 CD86 的增加。MCC950 减轻了 AKI 后 CD11c+细胞的激活并改善了肾功能。总之,使用 MPM 或 LSFM 结合肾脏透明化进行广泛而深入的三维可视化揭示了肾脏 MNP 的动态变化,这些变化与 AKI 中的肾功能直接相关。
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