Sex-Specific Changes in Cardiac Function and Electrophysiology During Progression of Adenine-Induced Chronic Kidney Disease in Mice

Valentina Dargam, Anet Sanchez, Aashiya Kolengaden, Yency Perez, Rebekah Arias, Ana M Valentin Cabrera, Daniel Chaparro, Christopher Tarafa, Alexandra Coba, Nathan Yapaolo, Emily A Todd, Monique Monelle Williams, Lina A Shehadeh, Joshua D Hutcheson
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Abstract

BACKGROUND Chronic kidney disease (CKD) and cardiovascular disease (CVD) often co-exist and interact; however, notable sex-dependent differences are observed in how these conditions manifest and progress in parallel, despite men and women sharing similar risk factors. Identifying sex-specific diagnostic markers of cardiac structure and function throughout CKD progression could elucidate why the development and progression of these diseases differ by sex. METHODS AND RESULTS Adult, C57BL/6J male and female mice were subjected to a high-adenine (0.2%) diet throughout 12-weeks to induce CKD. Control mice were fed a normal chow diet. Every three weeks, electrocardiogram (ECG) and echocardiogram-based markers of cardiac physiology were evaluated. Adenine-induced CKD showed markers of left ventricular (LV) hypertrophy in male mice only. CKD males had markers indicative of LV systolic and diastolic dysfunction throughout regimen duration, worsening as disease progressed. Adenine males had a prolonged QTc and STc intervals when compared to Adenine females and Control males. Sex-dependent differences in the duration of the Speak-J marker, measured via ECG, was identified, with Adenine males showing increases in duration earlier than Adenine females compared to their Control counterparts. CONCLUSIONS In this study, we identified sex-dependent differences in cardiac structure, function, and electrophysiology in a mouse model of CKD-induced CVD throughout disease progression. We found that male mice are more prone to developing LV hypertrophy, systolic dysfunction, and diastolic dysfunction, with significant increases in ECG markers indicative of ventricular dysfunction observed in adenine-treated males at late stages of the disease. Additionally, we identified a new ECG parameter, Speak-J duration, that highlights sex-specific cardiac electrophysiological changes, demonstrating the model's utility in studying sex-dependent cardiac differences.
腺嘌呤诱导的小鼠慢性肾病进展过程中心功能和电生理学的性别特异性变化
背景慢性肾脏疾病(CKD)和心血管疾病(CVD)常常同时存在并相互作用;然而,尽管男性和女性具有相似的风险因素,但在这些疾病的表现和并行进展方面却观察到明显的性别差异。在 CKD 的整个进展过程中确定心脏结构和功能的性别特异性诊断标记物,可以阐明为什么这些疾病的发生和进展因性别而异。对照组小鼠食用正常饲料。每三周对心电图(ECG)和基于超声心动图的心脏生理指标进行一次评估。腺嘌呤诱导的 CKD 仅在雄性小鼠中显示出左心室肥大的标志物。在整个治疗过程中,CKD 雄性小鼠的左心室收缩和舒张功能障碍指标,随着病情的发展而恶化。与腺嘌呤雌鼠和对照组雄鼠相比,腺嘌呤雄鼠的 QTc 和 STc 间期延长。通过心电图测量发现,Speak-J 标记的持续时间存在性别差异,与对照组相比,腺嘌呤雄性小鼠比腺嘌呤雌性小鼠更早出现持续时间延长。我们发现雄性小鼠更容易出现左心室肥大、收缩功能障碍和舒张功能障碍,在疾病晚期,经腺嘌呤处理的雄性小鼠心电图标志物显著增加,表明心室功能障碍。此外,我们还发现了一个新的心电图参数--Speak-J持续时间,它能突出显示性别特异性的心脏电生理变化,证明了该模型在研究性别依赖性心脏差异方面的实用性。
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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