Conjoint Internal Medicine Laboratory, Chemical Pathology Pathology Queensland Brisbane Queensland Australia.
Kidney Health Service Royal Brisbane and Women's Hospital Brisbane Queensland Australia.
J Extracell Vesicles. 2021 Feb;10(4):e12064. doi: 10.1002/jev2.12064. Epub 2021 Feb 16.
Proximal tubular epithelial cells (PTEC) are central players in inflammatory kidney diseases. However, the complex signalling mechanism/s via which polarized PTEC mediate disease progression are poorly understood. Small extracellular vesicles (sEV), including exosomes, are recognized as fundamental components of cellular communication and signalling courtesy of their molecular cargo (lipids, microRNA, proteins). In this study, we examined the molecular content and function of sEV secreted from the apical versus basolateral surfaces of polarized human primary PTEC under inflammatory diseased conditions. PTEC were cultured under normal and inflammatory conditions on Transwell inserts to enable separate collection and isolation of apical/basolateral sEV. Significantly increased numbers of apical and basolateral sEV were secreted under inflammatory conditions compared with equivalent normal conditions. Multi-omics analysis revealed distinct molecular profiles (lipids, microRNA, proteins) between inflammatory and normal conditions for both apical and basolateral sEV. Biological pathway analyses of significantly differentially expressed molecules associated apical inflammatory sEV with processes of cell survival and immunological disease, while basolateral inflammatory sEV were linked to pathways of immune cell trafficking and cell-to-cell signalling. In line with this mechanistic concept, functional assays demonstrated significantly increased production of chemokines (monocyte chemoattractant protein-1, interleukin-8) and immuno-regulatory cytokine interleukin-10 by peripheral blood mononuclear cells activated with basolateral sEV derived from inflammatory PTEC. We propose that the distinct molecular composition of sEV released from the apical versus basolateral membranes of human inflammatory PTEC may reflect specialized functional roles, with basolateral-derived sEV pivotal in modulating tubulointerstitial inflammatory responses observed in many immune-mediated kidney diseases. These findings provide a rationale to further evaluate these sEV-mediated inflammatory pathways as targets for biomarker and therapeutic development.
近端肾小管上皮细胞 (PTEC) 是炎症性肾脏疾病的核心参与者。然而,极化的 PTEC 介导疾病进展的复杂信号机制仍知之甚少。小细胞外囊泡 (sEV),包括外泌体,由于其分子货物 (脂质、microRNA、蛋白质),被认为是细胞通讯和信号传递的基本组成部分。在这项研究中,我们研究了在炎症性疾病条件下极化的人原代 PTEC 从顶端到基底外侧表面分泌的 sEV 的分子内容和功能。PTEC 在 Transwell 插入物上在正常和炎症条件下培养,以分别收集和分离顶端/基底外侧 sEV。与等效的正常条件相比,炎症条件下分泌的顶端和基底外侧 sEV 数量明显增加。多组学分析显示,顶端和基底外侧 sEV 在炎症和正常条件下均具有不同的分子谱(脂质、microRNA、蛋白质)。与顶端炎症性 sEV 相关的显著差异表达分子的生物学途径分析与细胞存活和免疫性疾病过程相关,而基底外侧炎症性 sEV 与免疫细胞迁移和细胞间信号转导途径相关。与这一机制概念一致,功能测定表明,用源自炎症性 PTEC 的基底外侧 sEV 激活的外周血单核细胞产生的趋化因子(单核细胞趋化蛋白-1、白细胞介素-8)和免疫调节细胞因子白细胞介素-10 明显增加。我们提出,从人炎症性 PTEC 的顶侧和基底外侧膜释放的 sEV 的独特分子组成可能反映了专门的功能作用,基底外侧衍生的 sEV 在调节许多免疫介导的肾脏疾病中观察到的肾小管间质炎症反应中具有关键作用。这些发现为进一步评估这些 sEV 介导的炎症途径作为生物标志物和治疗开发的靶点提供了依据。
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