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确定源自近端肾小管的保护性肾缺血预处理的 microRNA 特征。

Determination of a microRNA signature of protective kidney ischemic preconditioning originating from proximal tubules.

机构信息

Wales Kidney Research Unit, School of Medicine, College of Biomedical & Life Sciences, Cardiff University, Heath Park Campus, Cardiff, CF14 4XN, UK.

Cardiff Transplant Unit, University Hospital of Wales, Cardiff, CF14 4XW, UK.

出版信息

Sci Rep. 2021 May 10;11(1):9862. doi: 10.1038/s41598-021-89195-3.

Abstract

Ischemic preconditioning (IPC) is effective in limiting subsequent ischemic acute kidney injury in experimental models. MicroRNAs are an important class of post-transcriptional regulator and show promise as biomarkers of kidney injury. We evaluated the time- and dose-dependence of benefit from IPC in a rat model of functional (bilateral) ischemia-reperfusion injury (IRI). We found optimal protection from subsequent injury following short, repetitive sequences of preconditioning insult. We subsequently used hybridization array and microRNA sequencing to characterize microRNA signatures of protective IPC and of IRI. These approaches identified a profile of microRNA changes consequent on IRI, that were limited by prior IPC. To localize these signals within the kidney, we used laser capture microdissection and RT-qPCR to measure microRNA abundance in nephron segments, pinpointing microRNA changes principally to glomeruli and proximal tubules. Our data describe a unique microRNA signature for IRI in the rat kidney. Pulsatile IPC reduces kidney damage following IRI and diminishes this microRNA signal. We have also identified candidate microRNAs that may act as biomarkers of injury and therapeutic targets in this context.

摘要

缺血预处理 (IPC) 在限制实验模型中随后发生的缺血性急性肾损伤方面是有效的。microRNAs 是一类重要的转录后调节剂,有望成为肾损伤的生物标志物。我们在大鼠功能性(双侧)缺血再灌注损伤 (IRI) 模型中评估了 IPC 获益的时间和剂量依赖性。我们发现,在短时间内进行重复预处理刺激后,对随后的损伤有最佳的保护作用。随后,我们使用杂交阵列和 microRNA 测序来描述保护性 IPC 和 IRI 的 microRNA 特征。这些方法确定了与 IRI 相关的 microRNA 变化的特征,这些变化受到先前 IPC 的限制。为了在肾脏内定位这些信号,我们使用激光捕获微切割和 RT-qPCR 来测量肾单位节段中的 microRNA 丰度,将 microRNA 变化主要定位在肾小球和近端肾小管。我们的数据描述了大鼠肾脏 IRI 的独特 microRNA 特征。脉动 IPC 可减少 IRI 后的肾脏损伤,并减弱这种 microRNA 信号。我们还鉴定了候选 microRNAs,它们可能在此类情况下作为损伤的生物标志物和治疗靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/59a2/8110756/83abdf093fb5/41598_2021_89195_Fig1_HTML.jpg

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