Acute kidney injury results in long-term alterations of kidney lymphatics in mice.

Gelare Ghajar-Rahimi, Daria Barwinska, Grace E Whipple, Malgorzata M Kamocka, Shehnaz Khan, Seth Winfree, Jennifer Lafontaine, Reham H Soliman, Arin L Melkonian, Anna A Zmijewska, Matthew D Cheung, Amie M Traylor, Yanlin Jiang, Zhengqin Yang, Subhashini Bolisetty, Abolfazl Zarjou, Timmy Lee, James F George, Tarek M El-Achkar, Anupam Agarwal
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Abstract

The long-term effects of a single episode of acute kidney injury (AKI) induced by bilateral ischemia-reperfusion injury (BIRI) on kidney lymphatic dynamics are not known. The purpose of this study was to determine if alterations in kidney lymphatics are sustained in the long term and how they relate to inflammation and injury. Mice underwent BIRI as a model of AKI and were followed up to 9 mo. Although kidney function markers normalized following initial injury, histological analysis revealed sustained tissue damage and inflammation for up to 9 mo. Transcriptional analysis showed both acute and late-stage lymphangiogenesis, supported by increased expression of lymphatic markers, with unique signatures at each phase. Expression of Ccl21a was distinctly upregulated during late-stage lymphangiogenesis. Three-dimensional tissue cytometry confirmed increased lymphatic vessel abundance, particularly in the renal cortex, at early and late timepoints postinjury. In addition, the study identified the formation of tertiary lymphoid structures composed of CCR7+ lymphocytes and observed changes in immune cell composition over time, suggesting a complex and dynamic response to AKI involving tissue remodeling and immune cell involvement. This study provides new insights into the role of lymphatics in the progression of AKI to chronic kidney disease.NEW & NOTEWORTHY Here, we perform the first, comprehensive study of long-term lymphatic dynamics following a single acute kidney injury (AKI) event. Using improved three-dimensional image analysis and an expanded panel of transcriptional markers, we identify multiple stages of lymphatic responses with distinct transcriptional signatures, associations with the immune microenvironment, and collagen deposition. This research advances kidney lymphatic biology, emphasizing the significance of longitudinal studies in understanding AKI and the transition to chronic kidney disease.

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急性肾损伤导致小鼠肾淋巴管的长期改变
由双侧缺血再灌注损伤(BIRI)诱发的单次急性肾损伤(AKI)对肾脏淋巴动力学的长期影响尚不清楚。本研究旨在确定肾脏淋巴管的改变是否会长期持续,以及它们与炎症和损伤之间的关系。小鼠接受了作为 AKI 模型的 BIRI,并接受了长达 9 个月的随访。虽然肾功能指标最初趋于正常,但组织学分析显示组织损伤和炎症持续时间长达9个月。转录分析表明,淋巴标志物的表达增加支持了急性和晚期淋巴管生成,每个阶段都有独特的特征。在晚期淋巴管生成过程中,Ccl21a的表达明显上调。三维组织细胞仪证实,在损伤后的早期和晚期时间点,淋巴管丰度增加,尤其是在肾皮质。此外,研究还确定了由 CCR7+ 淋巴细胞组成的三级淋巴结构的形成,并观察到免疫细胞组成随时间的变化,这表明对 AKI 的反应是复杂和动态的,涉及组织重塑和免疫细胞参与。这些研究为淋巴管在 AKI 进展为慢性肾病过程中的作用提供了新的见解。
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