Left Heart Abnormalities in Patients With Lung Disease, OSA, and Chronic Thromboemboli at Risk for or With Known Pulmonary Hypertension.

IF 7.8 1区医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS

Circulation: Heart Failure Pub Date : 2025-05-29 DOI:10.1161/CIRCHEARTFAILURE.125.012912

Yogesh N V Reddy, Robert P Frantz, Paul M Hassoun, Anna Hemnes, Evelyn Horn, Jane A Leopold, Franz Rischard, Erika B Rosenzweig, Nicholas S Hill, Serpil C Erzurum, Gerald J Beck, J Emanuel Finet, Christine L Jellis, Stephen C Mathai, Reena Mehra, W H Wilson Tang, Barry A Borlaug

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Abstract

Background: Patients with lung disease, sleep apnea, and chronic thromboemboli can develop pulmonary hypertension, currently classified as group 3 or 4. Many of these patients also have risk factors for heart failure with preserved ejection fraction (HFpEF), but the optimal approach to identify the disease overlap remains unclear.

Methods: Pretest probability for HFpEF was determined using the HFpEF-ABA algorithm among adjudicated group 3 or 4 patients at risk for pulmonary hypertension in the PVDOMICS study (Redefining Pulmonary Hypertension Through Pulmonary Vascular Disease Phenomics). Patients were stratified by current resting right heart catheterization criteria, and in a separate analysis, stratified only by HFpEF-ABA probability into low (<25%), intermediate, and high (≥75%) HFpEF probability groups.

Results: Among 598 patients with group 3 disease, 27% (n=161) had elevated pulmonary capillary wedge pressure (PCWP) with postcapillary pulmonary hypertension even at rest, which was associated with the highest exercise PCWP. However, regardless of this resting PCWP-based classification, a larger subset had intermediate-to-high HFpEF-ABA probabilities (32% [n=197] high and 57% [n=358] intermediate HFpEF probability). High HFpEF probability in group 3 disease was associated with higher resting and dynamic PCWP response to NO, fluid, and exercise (P<0.0001 for all). These changes were comparable with more traditionally defined HFpEF without pulmonary vascular disease (n=61) but less severe than those with combined precapillary and postcapillary pulmonary hypertension HFpEF (n=31; interaction P=0.006). Increasing HFpEF probability in group 3 disease was associated with worse left heart remodeling, quality of life, 6-minute walk distance, and peak VO₂ (P<0.0001 for all). Findings were replicated in group 4 disease (n=102).

Conclusions: Quantifying pretest probability for HFpEF in patients with sleep apnea, lung disease, or chronic thromboemboli identifies a progressive gradient for dynamic PCWP abnormalities with worse functional status and quality of life. These subclinical left heart abnormalities are not universally detectable by resting right heart catheterization alone and call for further study of whether strategies to prevent or treat HFpEF might improve functional status in these patients with high risk of occult HFpEF.

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患有肺部疾病、阻塞性睡眠呼吸暂停和慢性血栓栓塞或已知肺动脉高压危险患者的左心异常

背景：患有肺部疾病、睡眠呼吸暂停和慢性血栓栓塞的患者可发生肺动脉高压，目前分为第3组或第4组。这些患者中的许多人也有保留射血分数（HFpEF）心力衰竭的危险因素，但确定疾病重叠的最佳方法仍不清楚。方法：在PVDOMICS研究（通过肺血管疾病表型学重新定义肺动脉高压）中确定的第3组或第4组有肺动脉高压风险的患者中，使用HFpEF- aba算法确定HFpEF的预测概率。根据当前静息右心导管标准对患者进行分层，并在一项单独的分析中，仅通过HFpEF-ABA概率将患者分层为低(结果：在598例3组疾病患者中，27% （n=161）的患者即使在静息时也有肺毛细血管楔压（PCWP）升高并毛细血管后肺动脉高压，这与最高的运动PCWP相关。然而，不管这种基于静息pcwp的分类，更大的子集具有中高的HFpEF- aba概率（32% [n=197]高和57% [n=358]中等HFpEF概率）。3组患者HFpEF发生率高与静息和动态PCWP对NO、液体和运动的反应较高相关（PP=0.006）。3组患者HFpEF概率的增加与左心重构、生活质量、6分钟步行距离和VO2峰值的恶化相关。结论：量化睡眠呼吸暂停、肺病或慢性血栓栓塞患者HFpEF的预测概率，确定了动态PCWP异常与更差的功能状态和生活质量的递进梯度。这些亚临床左心异常不能通过静息右心导管单独检测到，需要进一步研究预防或治疗HFpEF的策略是否可以改善这些隐匿性HFpEF高风险患者的功能状态。

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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来源期刊

Circulation: Heart Failure 医学-心血管系统

CiteScore

12.90

自引率

3.10%

发文量

271

审稿时长

6-12 weeks

期刊介绍： Circulation: Heart Failure focuses on content related to heart failure, mechanical circulatory support, and heart transplant science and medicine. It considers studies conducted in humans or analyses of human data, as well as preclinical studies with direct clinical correlation or relevance. While primarily a clinical journal, it may publish novel basic and preclinical studies that significantly advance the field of heart failure.