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尿液中足细胞释放的迁移小体可作为早期足细胞损伤的指标。

Podocyte-Released Migrasomes in Urine Serve as an Indicator for Early Podocyte Injury.

作者信息

Liu Ying, Li Shan, Rong Weiwei, Zeng Caihong, Zhu Xiaodong, Chen Qilin, Li Limin, Liu Zhi-Hong, Zen Ke

机构信息

National Clinical Research Center of Kidney Diseases, Jinling Hospital, Nanjing University School of Medicine, Nanjing, China.

Jiangsu Engineering Research Center for MicroRNA Biotechnology, Nanjing University School of Life Sciences, Nanjing, China.

出版信息

Kidney Dis (Basel). 2020 Nov;6(6):422-433. doi: 10.1159/000511504. Epub 2020 Oct 23.

Abstract

BACKGROUND

Levels of urinary microvesicles, which are increased during various kidney injuries, have diagnostic potential for renal diseases. However, the significance of urinary microvesicles as a renal disease indicator is dampened by the difficulty to ascertain their cell source.

OBJECTIVES

The aim of this study was to demonstrate that podocytes can release migrasomes, a unique class of microvesicle with size ranging between 400 and 2,000 nm, and the urine level of migrasomes may serve as novel non-invasive biomarker for early podocyte injury.

METHOD

In this study, immunofluorescence labeling, electronic microscopy, nanosite, and sequential centrifugation were used to purify and analyze migrasomes.

RESULTS

Migrasomes released by podocytes differ from exosomes as they have different content and mechanism of release. Compared to podocytes, renal tubular cells secrete markedly less migrasomes. Moreover, secretion of migrasomes by human or murine podocytes was strongly augmented during podocyte injuries induced by LPS, puromycin amino nucleoside (PAN), or a high concentration of glucose (HG). LPS, PAN, or HG-induced podocyte migrasome release, however, was blocked by Rac-1 inhibitor. Strikingly, a higher level of podocyte migrasomes in urine was detected in mice with PAN-nephropathy than in control mice. In fact, increased urinary migrasome number was detected earlier than elevated proteinuria during PAN-nephropathy, suggesting that urinary migrasomes are a more sensitive podocyte injury indicator than proteinuria. Increased urinary migrasome number was also detected in diabetic nephropathy patients with proteinuria level <5.5 g/day.

CONCLUSIONS

Our findings reveal that podocytes release the "injury-related" migrasomes during migration and provide urinary podocyte migrasome as a potential diagnostic marker for early podocyte injury.

摘要

背景

尿微泡水平在各种肾损伤过程中会升高,对肾脏疾病具有诊断潜力。然而,尿微泡作为肾脏疾病指标的意义因难以确定其细胞来源而受到影响。

目的

本研究旨在证明足细胞可释放迁移体,这是一类独特的微泡,大小在400至2000纳米之间,且尿液中迁移体水平可作为早期足细胞损伤的新型非侵入性生物标志物。

方法

在本研究中,采用免疫荧光标记、电子显微镜、纳米位点和连续离心法来纯化和分析迁移体。

结果

足细胞释放的迁移体与外泌体不同,因为它们具有不同的内容物和释放机制。与足细胞相比,肾小管细胞分泌的迁移体明显较少。此外,在脂多糖、嘌呤霉素氨基核苷(PAN)或高浓度葡萄糖(HG)诱导的足细胞损伤过程中,人或小鼠足细胞迁移体的分泌显著增加。然而,脂多糖、PAN或HG诱导的足细胞迁移体释放被Rac-1抑制剂阻断。令人惊讶的是,与对照小鼠相比,PAN肾病小鼠尿液中的足细胞迁移体水平更高。事实上,在PAN肾病期间,尿液中迁移体数量增加的检测早于蛋白尿升高,这表明尿液中的迁移体是比蛋白尿更敏感的足细胞损伤指标。在蛋白尿水平<5.5 g/天的糖尿病肾病患者中也检测到尿液中迁移体数量增加。

结论

我们的研究结果表明,足细胞在迁移过程中释放“损伤相关”的迁移体,并提供尿液足细胞迁移体作为早期足细胞损伤的潜在诊断标志物。

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