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内皮细胞在心脏损伤过程中呈现出一种有利于修复的免疫应答特征。

Endothelial cells adopt a pro-reparative immune responsive signature during cardiac injury.

机构信息

https://ror.org/02pttbw34 Interdepartmental Program in Integrative Molecular and Biomedical Sciences, Baylor College of Medicine, Houston, TX, USA.

https://ror.org/02pttbw34 Department of Integrative Physiology, Baylor College of Medicine, Houston, TX, USA.

出版信息

Life Sci Alliance. 2023 Nov 27;7(2). doi: 10.26508/lsa.202201870. Print 2024 Feb.

Abstract

Modulation of the heart's immune microenvironment is crucial for recovery after ischemic events such as myocardial infarction (MI). Endothelial cells (ECs) can have immune regulatory functions; however, interactions between ECs and the immune environment in the heart after MI remain poorly understood. We identified an EC-specific IFN responsive and immune regulatory gene signature in adult and pediatric heart failure (HF) tissues. Single-cell transcriptomic analysis of murine hearts subjected to MI uncovered an EC population (IFN-ECs) with immunologic gene signatures similar to those in human HF. IFN-ECs were enriched in regenerative-stage mouse hearts and expressed genes encoding immune responsive transcription factors (, , and ). Single-cell chromatin accessibility studies revealed an enrichment of these TF motifs at IFN-EC signature genes. Expression of immune regulatory ligand genes by IFN-ECs suggests bidirectional signaling between IFN-ECs and macrophages in regenerative-stage hearts. Our data suggest that ECs may adopt immune regulatory signatures after cardiac injury to accompany the reparative response. The presence of these signatures in human HF and murine MI models suggests a potential role for EC-mediated immune regulation in responding to stress induced by acute injury in MI and chronic adverse remodeling in HF.

摘要

调节心脏的免疫微环境对于缺血事件(如心肌梗死)后的恢复至关重要。内皮细胞(EC)具有免疫调节功能;然而,心肌梗死后 EC 与心脏免疫环境之间的相互作用仍知之甚少。我们在成人和儿科心力衰竭(HF)组织中鉴定出一种 EC 特异性 IFN 反应和免疫调节基因特征。对接受 MI 的鼠心进行单细胞转录组分析,揭示了一种具有与人类 HF 相似免疫基因特征的 EC 群体(IFN-ECs)。IFN-ECs 在再生阶段的鼠心中富集,并表达编码免疫反应性转录因子(、、和)的基因。单细胞染色质可及性研究显示,这些 TF 基序在 IFN-EC 特征基因中富集。IFN-EC 表达免疫调节配体基因,提示 IFN-ECs 和巨噬细胞之间在再生阶段心脏中存在双向信号转导。我们的数据表明,EC 可能在心脏损伤后采用免疫调节特征,以伴随修复反应。这些特征在人类 HF 和鼠 MI 模型中的存在表明,EC 介导的免疫调节在 MI 中的急性损伤和 HF 中的慢性不良重塑所引起的应激中可能发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/052d/10681909/ded46c5a6172/LSA-2022-01870_Fig1.jpg

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