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肾闰细胞全转录组分析预测脂多糖介导的视黄酸 X 受体 α 功能抑制。

Whole Transcriptome Analysis of Renal Intercalated Cells Predicts Lipopolysaccharide Mediated Inhibition of Retinoid X Receptor alpha Function.

机构信息

Indiana University School of Medicine, Riley Children's Hospital, Indianapolis, Indiana, United States.

The Institute for Genomic Medicine, Nationwide Children's Hospital, Columbus, Ohio, United States.

出版信息

Sci Rep. 2019 Jan 24;9(1):545. doi: 10.1038/s41598-018-36921-z.

Abstract

The renal collecting duct consists of intercalated cells (ICs) and principal cells (PCs). We have previously demonstrated that collecting ducts have a role in the innate immune defense of the kidney. Transcriptomics is an important tool used to enhance systems-level understanding of cell biology. However, transcriptomics performed on whole kidneys provides limited insight of collecting duct cell gene expression, because these cells comprise a small fraction of total kidney cells. Recently we generated reporter mouse models to enrich collecting duct specific PC and ICs and reported targeted gene expression of anti-microbial peptide genes. Here we report transcriptomics on enriched ICs and PCs and performed a pilot study sequencing four single ICs. We identified 3,645 genes with increased relative expression in ICs compared to non-ICs. In comparison to non-PCs, 2,088 genes had higher relative expression in PCs. IC associated genes included the innate interleukin 1 receptor, type 1 and the antimicrobial peptide(AMP) adrenomedullin. The top predicted canonical pathway for enriched ICs was lipopolysaccharide/Interleukin 1 mediated inhibition of Retinoid X Receptor alpha function and decreased Retinoid X Receptor expression was confirmed to occur 1-hour post experimental murine UTI in ICs but not in non-ICs.

摘要

肾集合管由闰细胞(ICs)和主细胞(PCs)组成。我们之前已经证明,集合管在肾脏的固有免疫防御中起作用。转录组学是一种用于增强细胞生物学系统水平理解的重要工具。然而,对整个肾脏进行转录组学分析只能提供对集合管细胞基因表达的有限了解,因为这些细胞仅占肾脏细胞总数的一小部分。最近,我们生成了报告小鼠模型以富集特定的集合管 PC 和 IC,并报道了靶向抗菌肽基因的表达。在这里,我们报告了富集的 IC 和 PCs 的转录组学,并对四个单个 IC 进行了测序的初步研究。我们在 IC 中鉴定出了 3645 个与非 IC 相比相对表达增加的基因。与非 PCs 相比,2088 个基因在 PCs 中的相对表达更高。与 IC 相关的基因包括先天白细胞介素 1 受体,1 型和抗菌肽(AMP)肾上腺髓质素。富集 IC 的顶级预测经典途径是脂多糖/白细胞介素 1 介导的视黄酸受体α功能抑制和视黄酸受体表达减少,在实验性小鼠尿路感染后 1 小时在 IC 中而不是非 IC 中证实发生。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1285/6345901/f46f1840f529/41598_2018_36921_Fig1_HTML.jpg

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