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胎儿中期伴有心肌结构紊乱的复杂先天性心脏病。

Complex Congenital Heart Disease Associated With Disordered Myocardial Architecture in a Midtrimester Human Fetus.

机构信息

Institute of Cardiovascular Science (P.G.-C., A.C.C.), University College London, United Kingdom.

Department of Information and Communications Technologies, Universitat Pompeu Fabra, Barcelona, Spain (P.G.-C., C.Z., C.B., B.B.).

出版信息

Circ Cardiovasc Imaging. 2018 Oct;11(10):e007753. doi: 10.1161/CIRCIMAGING.118.007753.

Abstract

BACKGROUND

In the era of increasingly successful corrective interventions in patients with congenital heart disease (CHD), global and regional myocardial remodeling are emerging as important sources of long-term morbidity/mortality. Changes in organization of the myocardium in CHD, and in its mechanical properties, conduction, and blood supply, result in altered myocardial function both before and after surgery. To gain a better understanding and develop appropriate and individualized treatment strategies, the microscopic organization of cardiomyocytes, and their integration at a macroscopic level, needs to be completely understood. The aim of this study is to describe, for the first time, in 3 dimensions and nondestructively the detailed remodeling of cardiac microstructure present in a human fetal heart with complex CHD.

METHODS AND RESULTS

Synchrotron X-ray phase-contrast imaging was used to image an archival midgestation formalin-fixed fetal heart with right isomerism and complex CHD and compare with a control fetal heart. Analysis of myocyte aggregates, at detail not accessible with other techniques, was performed. Macroanatomic and conduction system changes specific to the disease were clearly observable, together with disordered myocyte organization in the morphologically right ventricle myocardium. Electrical activation simulations suggested altered synchronicity of the morphologically right ventricle.

CONCLUSIONS

We have shown the potential of X-ray phase-contrast imaging for studying cardiac microstructure in the developing human fetal heart at high resolution providing novel insight while preserving valuable archival material for future study. This is the first study to show myocardial alterations occur in complex CHD as early as midgestation.

摘要

背景

在先天性心脏病(CHD)患者的矫正干预日益成功的时代,全球和区域性心肌重构正在成为长期发病率/死亡率的重要来源。CHD 中心肌组织及其机械性能、传导和血液供应的变化导致手术前后心肌功能发生改变。为了更好地理解并制定适当和个体化的治疗策略,需要完全了解心肌细胞的微观结构及其在宏观水平上的整合。本研究的目的是首次在 3 维空间中对患有复杂 CHD 的人类胎儿心脏中的心脏微观结构进行详细的重构进行描述。

方法和结果

同步加速器 X 射线相衬成像用于对具有右位异构和复杂 CHD 的中孕期福尔马林固定胎儿心脏进行成像,并与对照胎儿心脏进行比较。对肌细胞聚集体进行了分析,这些聚集体是其他技术无法获得的细节。可明显观察到与疾病相关的宏观解剖和传导系统变化,以及形态右心室心肌中紊乱的肌细胞组织。电激活模拟表明形态右心室的同步性发生改变。

结论

我们已经证明了 X 射线相衬成像在高分辨率下研究人类胎儿心脏发育中心肌微观结构的潜力,在保留有价值的存档材料供未来研究的同时提供了新的见解。这是首次显示复杂 CHD 早在中孕期就出现心肌改变的研究。

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