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赋予人工智能以单细胞分辨率描绘人类心脏主起搏点的能力。

Empowering artificial intelligence in characterizing the human primary pacemaker of the heart at single cell resolution.

机构信息

Division of Cardiovascular Sciences, Faculty of Biology, Medicine and Health, The University of Manchester, Manchester, M13 9PL, UK.

Department of Anatomy, Jagiellonian University Medical College, 31-008, Kraków, Poland.

出版信息

Sci Rep. 2024 Jun 18;14(1):14041. doi: 10.1038/s41598-024-63542-6.

Abstract

The sinus node (SN) serves as the primary pacemaker of the heart and is the first component of the cardiac conduction system. Due to its anatomical properties and sample scarcity, the cellular composition of the human SN has been historically challenging to study. Here, we employed a novel deep learning deconvolution method, namely Bulk2space, to characterise the cellular heterogeneity of the human SN using existing single-cell datasets of non-human species. As a proof of principle, we used Bulk2Space to profile the cells of the bulk human right atrium using publicly available mouse scRNA-Seq data as a reference. 18 human cell populations were identified, with cardiac myocytes being the most abundant. Each identified cell population correlated to its published experimental counterpart. Subsequently, we applied the deconvolution to the bulk transcriptome of the human SN and identified 11 cell populations, including a population of pacemaker cardiomyocytes expressing pacemaking ion channels (HCN1, HCN4, CACNA1D) and transcription factors (SHOX2 and TBX3). The connective tissue of the SN was characterised by adipocyte and fibroblast populations, as well as key immune cells. Our work unravelled the unique single cell composition of the human SN by leveraging the power of a novel machine learning method.

摘要

窦房结 (SN) 是心脏的主要起搏点,也是心脏传导系统的第一个组成部分。由于其解剖学特性和样本稀缺性,人类 SN 的细胞组成一直难以研究。在这里,我们使用了一种新颖的深度学习去卷积方法,即 Bulk2space,利用现有的非人类物种的单细胞数据集来描述人类 SN 的细胞异质性。作为原理验证,我们使用 Bulk2space 使用公开的小鼠 scRNA-Seq 数据作为参考,对批量人类右心房的细胞进行分析。鉴定出 18 个人类细胞群,其中心肌细胞最为丰富。每个鉴定出的细胞群都与已发表的实验对应物相关。随后,我们将去卷积应用于人类 SN 的批量转录组,并鉴定出 11 个细胞群,包括表达起搏离子通道 (HCN1、HCN4、CACNA1D) 和转录因子 (SHOX2 和 TBX3) 的起搏心肌细胞群。SN 的结缔组织由脂肪细胞和成纤维细胞群以及关键的免疫细胞组成。我们的工作通过利用一种新颖的机器学习方法的力量,揭示了人类 SN 的独特单细胞组成。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7b2b/11189420/27b0fdf213f5/41598_2024_63542_Fig1_HTML.jpg

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