Myosin-based contraction is not necessary for cardiac c-looping in the chick embryo.

Anatomy and Embryology Pub Date : 2006-10-01 Epub Date: 2006-04-25 DOI:10.1007/s00429-006-0094-0
Mathieu C Rémond, Judy A Fee, Elliot L Elson, Larry A Taber
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引用次数: 31

Abstract

During the initial phase of cardiac looping, known as c-looping, the heart bends and twists into a c-shaped tube with the convex outer curvature normally directed toward the right side of the embryo. Despite intensive study for more than 80 years, the biophysical mechanisms that drive and regulate looping remain poorly understood, although some investigators have speculated that differential cytoskeletal contraction supplies the driving force for c-looping. The purpose of this investigation was to test this hypothesis. To inhibit contraction, embryonic chick hearts at stages 10-12 (10-16 somites, 33-48 h) were exposed to the myosin inhibitors 2,3-butanedione monoxime (BDM), ML-7, Y-27632, and blebbistatin. Experiments were conducted in both whole embryo culture and, to focus on bending alone, isolated heart culture. Measurements of heart stiffness and phosphorylation of the myosin regulatory light chains showed that BDM, Y-27632, and blebbistatin significantly reduced myocardial contractility, while ML-7 had a lesser effect. None of these drugs significantly affected looping during the studied stages. These results suggest that active contraction is not required for normal c-looping of the embryonic chick heart between stages 10 and 12.

基于肌球蛋白的收缩不是鸡胚心脏c-环形成所必需的。
在心脏环的初始阶段,称为c型环,心脏弯曲并扭曲成一个c型管,其外凸曲率通常指向胚胎的右侧。尽管经过80多年的深入研究,驱动和调节c环的生物物理机制仍然知之甚少,尽管一些研究者推测差异细胞骨架收缩提供了c环的驱动力。这项调查的目的是为了检验这一假设。为了抑制收缩,将10-12期(10-16个体点,33-48 h)的小鸡胚胎心脏暴露于肌球蛋白抑制剂2,3-丁二酮单肟(BDM)、ML-7、Y-27632和blebbistatin中。实验进行了全胚培养和单独弯曲离体心脏培养。心脏僵硬度和肌球蛋白调节轻链磷酸化的测量显示,BDM、Y-27632和blebbistatin显著降低心肌收缩力,而ML-7的作用较小。在研究阶段,这些药物都没有显著影响环。这些结果表明,在第10 ~ 12期,鸡胚心脏正常的c-环形成不需要主动收缩。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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