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慢性肾脏病的心脏影像标志物。

Cardiac Imaging Biomarkers in Chronic Kidney Disease.

机构信息

Department of Cardiology, University Hospital La Paz, 28046 Madrid, Spain.

Cardiology Unit, Madre Giuseppina Vannini Hospital, 00177 Rome, Italy.

出版信息

Biomolecules. 2023 Apr 29;13(5):773. doi: 10.3390/biom13050773.

Abstract

Uremic cardiomyopathy (UC), the peculiar cardiac remodeling secondary to the systemic effects of renal dysfunction, is characterized by left ventricular (LV) diffuse fibrosis with hypertrophy (LVH) and stiffness and the development of heart failure and increased rates of cardiovascular mortality. Several imaging modalities can be used to obtain a non-invasive assessment of UC by different imaging biomarkers, which is the focus of the present review. Echocardiography has been largely employed in recent decades, especially for the determination of LVH by 2-dimensional imaging and diastolic dysfunction by pulsed-wave and tissue Doppler, where it retains a robust prognostic value; more recent techniques include parametric assessment of cardiac deformation by speckle tracking echocardiography and the use of 3D-imaging. Cardiac magnetic resonance (CMR) imaging allows a more accurate assessment of cardiac dimensions, including the right heart, and deformation by feature-tracking imaging; however, the most evident added value of CMR remains tissue characterization. T1 mapping demonstrated diffuse fibrosis in CKD patients, increasing with the worsening of renal disease and evident even in early stages of the disease, with few, but emerging, prognostic data. Some studies using T2 mapping highlighted the presence of subtle, diffuse myocardial edema. Finally, computed tomography, though rarely used to specifically assess UC, might provide incidental findings carrying prognostic relevance, including information on cardiac and vascular calcification. In summary, non-invasive cardiovascular imaging provides a wealth of imaging biomarkers for the characterization and risk-stratification of UC; integrating results from different imaging techniques can aid a better understanding of the physiopathology of UC and improve the clinical management of patients with CKD.

摘要

尿毒症性心肌病(UC)是由肾功能障碍的全身效应引起的特殊心脏重构,其特征为左心室(LV)弥漫性纤维化伴肥厚(LVH)和僵硬,并发展为心力衰竭和心血管死亡率增加。几种成像方式可用于通过不同的成像生物标志物对 UC 进行非侵入性评估,这是本综述的重点。在最近几十年中,超声心动图得到了广泛应用,特别是用于通过二维成像确定 LVH 和通过脉冲波和组织多普勒确定舒张功能障碍,在这方面它仍然具有强大的预后价值;最近的技术包括斑点追踪超声心动图对心脏变形的参数评估和 3D 成像的使用。心脏磁共振(CMR)成像可更准确地评估心脏尺寸,包括右心,并通过特征追踪成像评估变形;然而,CMR 的最明显的附加值仍然是组织特征。T1 映射在 CKD 患者中显示弥漫性纤维化,随着肾脏疾病的恶化而增加,甚至在疾病的早期阶段就已经明显,虽然有一些但仍处于新兴阶段的预后数据。一些使用 T2 映射的研究强调了存在微妙的弥漫性心肌水肿。最后,计算机断层扫描虽然很少用于专门评估 UC,但可能会提供具有预后相关性的偶然发现,包括关于心脏和血管钙化的信息。总之,非侵入性心血管成像为 UC 的特征和风险分层提供了丰富的成像生物标志物;整合来自不同成像技术的结果可以帮助更好地了解 UC 的病理生理学,并改善 CKD 患者的临床管理。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2729/10216582/0c2756594a33/biomolecules-13-00773-g001.jpg

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