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斑马鱼小梁形成过程中心肌细胞行为的调控由 Neuregulin 2a 信号通路介导。

Regulation of cardiomyocyte behavior in zebrafish trabeculation by Neuregulin 2a signaling.

机构信息

Department of Developmental Genetics, Max Planck Institute for Heart and Lung Research, 61231 Bad Nauheim, Germany.

出版信息

Nat Commun. 2017 May 9;8:15281. doi: 10.1038/ncomms15281.

Abstract

Trabeculation is crucial for cardiac muscle growth in vertebrates. This process requires the Erbb2/4 ligand Neuregulin (Nrg), secreted by the endocardium, as well as blood flow/cardiac contractility. Here, we address two fundamental, yet unresolved, questions about cardiac trabeculation: why does it initially occur in the ventricle and not the atrium, and how is it modulated by blood flow/contractility. Using loss-of-function approaches, we first show that zebrafish Nrg2a is required for trabeculation, and using a protein-trap line, find that it is expressed in both cardiac chambers albeit with different spatiotemporal patterns. Through gain-of-function experiments, we show that atrial cardiomyocytes can also respond to Nrg2a signalling, suggesting that the cardiac jelly, which remains prominent in the atrium, represents a barrier to Erbb2/4 activation. Furthermore, we find that blood flow/contractility is required for Nrg2a expression, and that while non-contractile hearts fail to trabeculate, non-contractile cardiomyocytes are also competent to respond to Nrg2a/Erbb2 signalling.

摘要

小梁化对于脊椎动物的心肌生长至关重要。这个过程需要由心内膜分泌的 Erbb2/4 配体神经调节蛋白(Nrg),以及血流/心脏收缩力。在这里,我们解决了关于心脏小梁化的两个基本但尚未解决的问题:为什么它最初发生在心室而不是心房,以及血流/收缩力如何调节它。通过功能丧失方法,我们首先表明斑马鱼 Nrg2a 对于小梁化是必需的,并且使用蛋白陷阱系,发现它在心腔中均有表达,尽管具有不同的时空模式。通过功能获得实验,我们表明心房心肌细胞也可以对 Nrg2a 信号作出反应,这表明在心房中仍然很突出的心脏胶可能代表 Erbb2/4 激活的障碍。此外,我们发现血流/收缩力对于 Nrg2a 的表达是必需的,并且虽然非收缩性心脏无法小梁化,但非收缩性心肌细胞也能够对 Nrg2a/Erbb2 信号作出反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0484/5477525/8bf1e3d7995f/ncomms15281-f1.jpg

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