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空间分辨转录组分析在雌性小鼠急性肾损伤模型中的应用。

Spatially Resolved Transcriptomic Analysis of Acute Kidney Injury in a Female Murine Model.

机构信息

Division of Nephrology, Department of Medicine, Washington University in St. Louis, St. Louis, Missouri.

Department of Pathology and Immunology, Washington University in St. Louis, St. Louis, Missouri.

出版信息

J Am Soc Nephrol. 2022 Feb;33(2):279-289. doi: 10.1681/ASN.2021081150. Epub 2021 Dec 1.

Abstract

BACKGROUND

Single-cell sequencing technologies have advanced our understanding of kidney biology and disease, but the loss of spatial information in these datasets hinders our interpretation of intercellular communication networks and regional gene expression patterns. New spatial transcriptomic sequencing platforms make it possible to measure the topography of gene expression at genome depth.

METHODS

We optimized and validated a female bilateral ischemia-reperfusion injury model. Using the 10× Genomics Visium Spatial Gene Expression solution, we generated spatial maps of gene expression across the injury and repair time course, and applied two open-source computational tools, Giotto and SPOTlight, to increase resolution and measure cell-cell interaction dynamics.

RESULTS

An ischemia time of 34 minutes in a female murine model resulted in comparable injury to 22 minutes for males. We report a total of 16,856 unique genes mapped across our injury and repair time course. Giotto, a computational toolbox for spatial data analysis, enabled increased resolution mapping of genes and cell types. Using a seeded nonnegative matrix regression (SPOTlight) to deconvolute the dynamic landscape of cell-cell interactions, we found that injured proximal tubule cells were characterized by increasing macrophage and lymphocyte interactions even 6 weeks after injury, potentially reflecting the AKI to CKD transition.

CONCLUSIONS

In this transcriptomic atlas, we defined region-specific and injury-induced loss of differentiation markers and their re-expression during repair, as well as region-specific injury and repair transcriptional responses. Lastly, we created an interactive data visualization application for the scientific community to explore these results (http://humphreyslab.com/SingleCell/).

摘要

背景

单细胞测序技术提高了我们对肾脏生物学和疾病的认识,但这些数据集丢失了空间信息,这阻碍了我们对细胞间通讯网络和区域基因表达模式的解释。新的空间转录组测序平台使我们有可能在全基因组深度测量基因表达的地形。

方法

我们优化并验证了一个雌性双侧缺血再灌注损伤模型。我们使用 10× Genomics Visium 空间基因表达解决方案,生成了损伤和修复时间过程中基因表达的空间图谱,并应用了两个开源计算工具 Giotto 和 SPOTlight,以提高分辨率并测量细胞-细胞相互作用动态。

结果

在雌性鼠模型中,缺血 34 分钟导致的损伤与雄性的 22 分钟相似。我们报告了总共 16856 个独特的基因映射到我们的损伤和修复时间过程中。Giotto 是一个空间数据分析的计算工具箱,它可以实现基因和细胞类型分辨率更高的图谱。使用基于种子的非负矩阵回归(SPOTlight)来分解细胞-细胞相互作用的动态景观,我们发现,即使在损伤后 6 周,受损的近端肾小管细胞的特征是巨噬细胞和淋巴细胞相互作用增加,这可能反映了 AKI 到 CKD 的转变。

结论

在这个转录组图谱中,我们定义了区域特异性和损伤诱导的分化标志物的丧失及其在修复过程中的重新表达,以及区域特异性损伤和修复转录反应。最后,我们为科学界创建了一个交互式数据可视化应用程序,以探索这些结果(http://humphreyslab.com/SingleCell/)。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7a15/8819997/ce27f94e46a4/ASN.2021081150absf1.jpg

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