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A single-nucleus RNA-sequencing pipeline to decipher the molecular anatomy and pathophysiology of human kidneys

机译:单核RNA测序管线以破译人肾的分子解剖和病理生理学

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Defining cellular and molecular identities within the kidney is necessary to understand its organization and function in health and disease. Here we demonstrate a reproducible method with minimal artifacts for single-nucleus Droplet-based RNA sequencing (snDrop-Seq) that we use to resolve thirty distinct cell populations in human adult kidney. We define molecular transition states along more than ten nephron segments spanning two major kidney regions. We further delineate cell type-specific expression of genes associated with chronic kidney disease, diabetes and hypertension, providing insight into possible targeted therapies. This includes expression of a hypertension-associated mechano-sensory ion channel in mesangial cells, and identification of proximal tubule cell populations defined by pathogenic expression signatures. Our fully optimized, quality-controlled transcriptomic profiling pipeline constitutes a tool for the generation of healthy and diseased molecular atlases applicable to clinical samples.
机译:在肾脏内定义细胞和分子形式是理解其在健康和疾病中的组织和功能。在这里,我们证明了一种可重复的方法,其用于单核液滴基RNA测序(SNDrop-SEQ)的最小伪像,其用于解决人类成人肾脏中的三十个不同细胞群。我们沿着跨越两个主要肾脏区的十多个肾球段定义分子过渡状态。我们进一步描绘了与慢性肾病,糖尿病和高血压相关的基因的细胞类型特异性表达,提供了洞察力的靶向疗法。这包括在纱线细胞中表达高血压相关的机械感觉离子通道,以及鉴定由致病表达签名定义的近端小管细胞群。我们完全优化,质量控制的转录组分析管道构成了一种用于产生适用于临床样本的健康和患病分子壳种的工具。

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