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Circulating argonaute-bound microRNA-126 reports vascular dysfunction and treatment response in acute and chronic kidney disease

机译:循环的Argonaute-Bound MicroRNA-126在急性和慢性肾病中报告血管功能障碍和治疗反应

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摘要

Vascular and kidney dysfunction commonly co-exist. There is a need for biomarkers of vascular health. Circulating microRNAs are biomarkers; miR-126 is endothelial cell-enriched. We measured circulating miR-126 in rats with nephrotoxic nephritis (NTN) and humans with acute endothelial and renal injury (vasculitis associated with autoantibodies to neutrophil cytoplasm antigens (ANCAs)). We compared these findings to those from patients with chronic kidney disease (CKD) and end-stage renal disease (ESRD) and explored the relationship between miR-126 and vascular dysfunction. In NTN, miR-126 was reduced. In ANCA vasculitis (N = 70), pre-treatment miR-126 was reduced compared to health (N = 60) (88-fold). miR-126 increased 3.4-fold post-treatment but remained lower than in health (∼26-fold). Argonaute 2-bound miR-126 increased with ANCA vasculitis treatment. miR-126 did not differ between CKD (N = 30) and health but its concentration correlated with endothelial dysfunction. miR-126 was reduced in ESRD (N = 15) (∼350 fold). miR-126 may be a marker of vascular inflammation and could aid decision-making.
机译:血管和肾功能障碍通常共存。需要血管健康的生物标志物。循环的microRNA是生物标志物; miR-126是富含内皮细胞的。我们在肾毒性肾炎(NTN)和具有急性内皮和肾损伤的大鼠大鼠中测量循环miR-​​126(患有急性内皮和肾损伤(与中性粒细胞骨质抗原(ANCAS)相关的血管炎)。我们将这些发现与慢性肾病(CKD)和终末期肾病(ESRD)的结果进行了比较,并探讨了MiR-126和血管功能障碍之间的关系。在NTN中,MIR-126减少。在ANCA血管炎(n = 70)中,与健康(n = 60)(88倍)相比,预处理miR-126减少。 MiR-126后处理3.4倍,但仍然低于健康(〜26倍)。 Argonaute 2-Bound MiR-126随着ANCA血管炎治疗而增加。 MiR-126在CKD(n = 30)和健康之间没有区别,但其浓度与内皮功能障碍相关。 MIR-126在ESRD(n = 15)(〜350倍)中降低。 miR-126可以是血管炎症的标志物,可以帮助决策。

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