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Hand2在心脏神经嵴中的表达调节流出道和第二心脏场的发育。

Cardiac neural crest expression of Hand2 regulates outflow and second heart field development.

作者信息

Morikawa Yuka, Cserjesi Peter

机构信息

Department of Cell and Molecular Biology, Tulane University, New Orleans, LA 70118, USA.

出版信息

Circ Res. 2008 Dec 5;103(12):1422-9. doi: 10.1161/CIRCRESAHA.108.180083. Epub 2008 Nov 13.

Abstract

The cardiac neural crest (cNC) lineage plays key roles in heart development by directly contributing to heart structures and regulating development of other heart lineages. The basic helix-loop-helix factor Hand2 regulates development of cardiovascular structures and NC-derived tissues including those that contribute to face and peripheral nervous system. Although Hand2 is expressed in cNC, its role has not been examined because of an early embryonic lethality when Hand2 is deleted in the NC lineage. We find that the lethality is attributable to loss of norepinephrine synthesis that can be overcome by activating adrenergic receptors. In rescued embryos, loss of Hand2 in the NC lineage leads to the misalignment of the outflow tract and aortic arch arteries. Defects include pulmonary stenosis, interrupted aortic artery, retroesophageal right subclavian artery, and ventricular septum defect, which resemble congenital heart defects attributed to defects in the NC. Hand2 functions in part by regulating signaling from the cNC to other cardiac lineages but not by regulating migration or survival of the cNC. Loss of Hand2 in NC also uncovered a novel role for the cNC in regulating proliferation and differentiation of the second heart field-derived myocardium that persists late into development. These results show that the cNC functions as a major signaling center for heart development and Hand2 plays a pivotal role in regulating both cell-autonomous and -nonautonomous functions of the cNC.

摘要

心脏神经嵴(cNC)谱系通过直接参与心脏结构形成和调节其他心脏谱系的发育,在心脏发育中发挥关键作用。碱性螺旋-环-螺旋因子Hand2调节心血管结构以及神经嵴衍生组织的发育,这些组织包括对面部和周围神经系统有贡献的组织。虽然Hand2在cNC中表达,但其作用尚未得到研究,因为在神经嵴谱系中删除Hand2会导致早期胚胎致死。我们发现这种致死性归因于去甲肾上腺素合成的丧失,而激活肾上腺素能受体可以克服这一情况。在获救的胚胎中,神经嵴谱系中Hand2的缺失导致流出道和主动脉弓动脉排列不齐。缺陷包括肺动脉狭窄、主动脉中断、食管后右锁骨下动脉和室间隔缺损,这些类似于归因于神经嵴缺陷的先天性心脏缺陷。Hand2部分通过调节从cNC到其他心脏谱系的信号传导发挥作用,但不是通过调节cNC的迁移或存活。神经嵴中Hand2的缺失还揭示了cNC在调节第二心脏场衍生心肌的增殖和分化方面的新作用,这种作用在发育后期仍然存在。这些结果表明,cNC作为心脏发育的主要信号中心发挥作用,而Hand2在调节cNC的细胞自主和非自主功能方面发挥关键作用。

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