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人类扩张型和肥厚型心肌病的单细胞分析。

Single-nucleus profiling of human dilated and hypertrophic cardiomyopathy.

机构信息

Precision Cardiology Laboratory and the Cardiovascular Disease Initiative, The Broad Institute, Cambridge, MA, USA.

Precision Cardiology Laboratory, Bayer US LLC, Cambridge, MA, USA.

出版信息

Nature. 2022 Aug;608(7921):174-180. doi: 10.1038/s41586-022-04817-8. Epub 2022 Jun 22.

DOI:10.1038/s41586-022-04817-8
PMID:35732739
Abstract

Heart failure encompasses a heterogeneous set of clinical features that converge on impaired cardiac contractile function and presents a growing public health concern. Previous work has highlighted changes in both transcription and protein expression in failing hearts, but may overlook molecular changes in less prevalent cell types. Here we identify extensive molecular alterations in failing hearts at single-cell resolution by performing single-nucleus RNA sequencing of nearly 600,000 nuclei in left ventricle samples from 11 hearts with dilated cardiomyopathy and 15 hearts with hypertrophic cardiomyopathy as well as 16 non-failing hearts. The transcriptional profiles of dilated or hypertrophic cardiomyopathy hearts broadly converged at the tissue and cell-type level. Further, a subset of hearts from patients with cardiomyopathy harbour a unique population of activated fibroblasts that is almost entirely absent from non-failing samples. We performed a CRISPR-knockout screen in primary human cardiac fibroblasts to evaluate this fibrotic cell state transition; knockout of genes associated with fibroblast transition resulted in a reduction of myofibroblast cell-state transition upon TGFβ1 stimulation for a subset of genes. Our results provide insights into the transcriptional diversity of the human heart in health and disease as well as new potential therapeutic targets and biomarkers for heart failure.

摘要

心力衰竭涵盖了一组异质的临床特征,这些特征集中在心脏收缩功能受损上,是一个日益严重的公共健康问题。以前的工作强调了衰竭心脏中转录和蛋白质表达的变化,但可能忽略了不太常见的细胞类型中的分子变化。在这里,我们通过对 11 例扩张型心肌病和 15 例肥厚型心肌病以及 16 例非衰竭心脏的左心室样本中的近 600,000 个核进行单细胞 RNA 测序,以单细胞分辨率识别衰竭心脏中的广泛分子改变。扩张型或肥厚型心肌病心脏的转录谱在组织和细胞类型水平上广泛趋同。此外,一组来自心肌病患者的心脏存在一种独特的激活成纤维细胞群体,这种群体在非衰竭样本中几乎完全不存在。我们在原代人心肌成纤维细胞中进行了 CRISPR 敲除筛选,以评估这种成纤维细胞状态转变;对于一组基因,敲除与成纤维细胞转变相关的基因可减少 TGFβ1 刺激下肌成纤维细胞状态的转变。我们的研究结果为人类心脏在健康和疾病中的转录多样性提供了新的见解,并为心力衰竭提供了新的潜在治疗靶点和生物标志物。

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Generalizing RNA velocity to transient cell states through dynamical modeling.
心肌细胞中的Janus激酶1(JAK1)信号传导是心脏内环境稳态和细胞因子依赖性STAT3激活所必需的。
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Integrated MicroRNA-mRNA Sequencing Analysis Identifies Regulators and Networks Involved in Feline Hypertrophic Cardiomyopathy.整合的微小RNA-信使核糖核酸测序分析鉴定出参与猫肥厚性心肌病的调控因子和网络。
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