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非再生系统与再生系统中心肌梗死后白细胞介导的心脏修复

Leukocyte-Mediated Cardiac Repair after Myocardial Infarction in Non-Regenerative vs. Regenerative Systems.

作者信息

Peterson Elizabeth Anne, Sun Jisheng, Wang Jinhu

机构信息

Division of Cardiology, School of Medicine, Emory University, Atlanta, GA 30322, USA.

出版信息

J Cardiovasc Dev Dis. 2022 Feb 21;9(2):63. doi: 10.3390/jcdd9020063.

Abstract

Innate and adaptive leukocytes rapidly mobilize to ischemic tissues after myocardial infarction in response to damage signals released from necrotic cells. Leukocytes play important roles in cardiac repair and regeneration such as inflammation initiation and resolution; the removal of dead cells and debris; the deposition of the extracellular matrix and granulation tissue; supporting angiogenesis and cardiomyocyte proliferation; and fibrotic scar generation and resolution. By organizing and comparing the present knowledge of leukocyte recruitment and function after cardiac injury in non-regenerative to regenerative systems, we propose that the leukocyte response to cardiac injury differs in non-regenerative adult mammals such as humans and mice in comparison to cardiac regenerative models such as neonatal mice and adult zebrafish. Specifically, extensive neutrophil, macrophage, and T-cell persistence contributes to a lengthy inflammatory period in non-regenerative systems for adverse cardiac remodeling and heart failure development, whereas their quick removal supports inflammation resolution in regenerative systems for new contractile tissue formation and coronary revascularization. Surprisingly, other leukocytes have not been examined in regenerative model systems. With this review, we aim to encourage the development of improved immune cell markers and tools in cardiac regenerative models for the identification of new immune targets in non-regenerative systems to develop new therapies.

摘要

心肌梗死后,固有免疫细胞和适应性免疫细胞会迅速响应坏死细胞释放的损伤信号,向缺血组织动员。白细胞在心脏修复和再生中发挥重要作用,如启动和消退炎症;清除死亡细胞和碎片;沉积细胞外基质和肉芽组织;支持血管生成和心肌细胞增殖;以及生成和消退纤维化瘢痕。通过整理和比较目前关于非再生系统到再生系统中心脏损伤后白细胞募集和功能的知识,我们提出,与新生小鼠和成年斑马鱼等心脏再生模型相比,在人类和小鼠等非再生成年哺乳动物中,白细胞对心脏损伤的反应有所不同。具体而言,在非再生系统中,大量中性粒细胞、巨噬细胞和T细胞的持续存在导致炎症期延长,从而引发不良的心脏重塑和心力衰竭,而在再生系统中,它们的快速清除有助于炎症消退,促进新的收缩组织形成和冠状动脉再血管化。令人惊讶的是,在再生模型系统中尚未对其他白细胞进行研究。通过本综述,我们旨在鼓励在心脏再生模型中开发改进的免疫细胞标记物和工具,以识别非再生系统中的新免疫靶点,从而开发新的治疗方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d3b1/8877434/235e99244dbf/jcdd-09-00063-g001.jpg

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