Department of Obstetrics and Gynecology, Division of Maternal Fetal Medicine, Chiang Mai University, Chiang Mai, Thailand.
Cardiac Electrophysiology Research and Training Center (CERT), Faculty of Medicine, Chiang Mai University, Chiang Mai, Thailand.
BMC Pregnancy Childbirth. 2024 Feb 16;24(1):141. doi: 10.1186/s12884-023-06232-x.
Whether or not the effects of anemia in the early phase, while the fetuses attempts to increase cardiac output to meet oxygen requirement in peripheral organs, is detrimental to the fetal developing vital organs is little-known. The objective of this is to compare prenatal cardiovascular changes and post-abortal cellular damages in the myocardium as a pumping organ and the brain as a perfused organ between anemic fetuses (using fetal Hb Bart's disease as a study model) in pre-hydropic phase and non-anemic fetuses.
Fetuses affected by Hb Bart's disease and non-anemic fetuses at 16-22 weeks were recruited to undergo comprehensive fetal echocardiography. Cord blood analysis was used to confirm the definite diagnosis of fetal Hb Bart's disease and normal fetuses. Fetal cardiac and brain tissues were collected shortly after pregnancy termination for the determination of oxidative stress and mitochondrial function, including mitochondrial ROS production and mitochondrial membrane changes.
A total of 18 fetuses affected by Hb Bart's disease and 13 non-anemic fetuses were recruited. The clinical characteristics of both groups were comparable. The affected fetuses showed a significant increase in cardiac dimensions, cardiac function, cardiac output and brain circulation without deteriorating cardiac contractility and preload. However, in the affected fetuses, mitochondrial dysfunction was clearly demonstrated in brain tissues and in the myocardium, as indicated by a significant increase in the membrane potential change (p-value < 0.001), and a significant increase in ROS production in brain tissues, with a trend to increase in myocardium. The findings indicated cellular damage in spite of good clinical compensation.
The new insight is that, in response to fetal anemia, fetal heart increases in size (dilatation) and function to increase cardiac output and blood flow velocity to provide adequate tissue perfusion, especially brain circulation. However, the myocardium and brain showed a significant increase in mitochondrial dysfunction, suggesting cellular damage secondary to anemic hypoxia. The compensatory increase in circulation could not completely prevent subtle brain and heart damage.
在胎儿试图增加心输出量以满足外周器官的氧气需求的早期阶段,贫血对胎儿发育重要器官的影响是否有害尚不清楚。本研究旨在比较处于预水肿期的贫血胎儿(以胎儿 Hb Bart's 病为研究模型)和非贫血胎儿的产前心血管变化和心肌作为泵器官和脑作为灌注器官的流产后细胞损伤。
招募 16-22 周受 Hb Bart's 病影响的胎儿和非贫血胎儿进行全面胎儿超声心动图检查。通过脐血分析确认胎儿 Hb Bart's 病和正常胎儿的明确诊断。妊娠终止后不久采集胎儿心脏和脑组织,用于测定氧化应激和线粒体功能,包括线粒体 ROS 产生和线粒体膜变化。
共纳入 18 例受 Hb Bart's 病影响的胎儿和 13 例非贫血胎儿。两组的临床特征相似。受影响的胎儿表现出心脏尺寸、心脏功能、心输出量和脑循环的显著增加,而不恶化心脏收缩力和前负荷。然而,在受影响的胎儿中,脑组织和心肌中线粒体功能障碍明显,表现为膜电位变化显著增加(p 值<0.001),脑组织 ROS 产生显著增加,心肌呈增加趋势。这些发现表明尽管有良好的临床代偿,但仍存在细胞损伤。
新的见解是,为了应对胎儿贫血,胎儿心脏增大(扩张)并增强功能以增加心输出量和血流速度,以提供足够的组织灌注,特别是脑循环。然而,心肌和大脑表现出明显的线粒体功能障碍,表明继发于贫血缺氧的细胞损伤。循环的代偿性增加并不能完全防止细微的脑和心脏损伤。
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