Myocardial inflammation is associated with impaired mitochondrial oxidative capacity in ischaemic cardiomyopathy.

IF 3.2 2区医学 Q2 CARDIAC & CARDIOVASCULAR SYSTEMS

ESC Heart Failure Pub Date : 2024-10-30 DOI:10.1002/ehf2.15133

Julius Borger, Elric Zweck, Constanze Moos, Patrick Horn, Fabian Voß, Heinz-Peter Schultheiss, Jacob Eifer Møller, Udo Boeken, Hug Aubin, Artur Lichtenberg, Malte Kelm, Michael Roden, Amin Polzin, Ralf Westenfeld, Julia Szendroedi, Daniel Scheiber

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引用次数: 0

Abstract

Aims: Myocardial inflammation and impaired mitochondrial oxidative capacity are hallmarks of heart failure (HF) pathophysiology. The extent of myocardial inflammation in patients suffering from ischaemic cardiomyopathy (ICM) or dilated cardiomyopathy (DCM) and its association with mitochondrial energy metabolism are unknown. We aimed at establishing a relevant role of cardiac inflammation in the impairment of mitochondrial energy production in advanced ischaemic and non-ischaemic HF.

Methods: We included 81 patients with stage D HF (ICM, n = 44; DCM, n = 37) undergoing left ventricular assist device implantation (n = 59) or heart transplantation (n = 22) and obtained left ventricular tissue samples during open heart surgery. We quantified mitochondrial oxidative capacity, citrate synthase activity (CSA) and fibrosis and lymphocytic infiltration. We considered infiltration of >14 CD3⁺ cells/mm² relevant inflammation.

Results: Patients with ICM or DCM did not differ regarding age (61.5 ± 5.7 vs. 56.5 ± 12.7 years, P = 0.164), sex (86% vs. 84% male, P = 0.725), type 2 diabetes mellitus (34% vs. 18%, P = 0.126) or chronic kidney disease (8% vs. 11%, P = 0.994). ICM exhibited oxidative capacity reduced by 23% compared to DCM (108.6 ± 41.4 vs. 141.9 ± 59.9 pmol/(s*mg), P = 0.006). Maximum production of reactive oxygen species was not significantly different between ICM and DCM (0.59 ± 0.28 vs. 0.69 ± 0.36 pmol/(s*ml), P = 0.196). Mitochondrial content, detected by CSA, was lower in ICM (359.6 ± 164.1 vs. 503.0 ± 198.5 nmol/min/mg protein, P = 0.002). Notably, relevant inflammation was more common in ICM (27% vs. 6%, P = 0.024), and the absolute number of infiltrating leucocytes correlated with lower oxidative capacity (r = -0.296, P = 0.019). Fibrosis was more prevalent in ICM (20.9 ± 21.2 vs. 7.2 ± 5.6% of area, P = 0.002), but not associated with oxidative capacity (r = -0.13, P = 0.327).

Conclusions: More than every fourth ICM patient with advanced HF displays myocardial inflammation in the range of inflammatory cardiomyopathy associated with reduced mitochondrial oxidative capacity. Future studies may evaluate inflammation in ICM at earlier stages in standardised fashion to explore the therapeutic potential of immunosuppression to influence trajectories of HF in ICM.

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心肌炎症与缺血性心肌病线粒体氧化能力受损有关。

目的：心肌炎症和线粒体氧化能力受损是心力衰竭（HF）病理生理学的标志。缺血性心肌病（ICM）或扩张型心肌病（DCM）患者心肌炎症的程度及其与线粒体能量代谢的关系尚不清楚。我们旨在确定心脏炎症在晚期缺血性和非缺血性高血压线粒体能量生成障碍中的相关作用：我们纳入了 81 名接受左心室辅助装置植入术（59 人）或心脏移植术（22 人）的 D 期高血压患者（ICM，44 人；DCM，37 人），并在开胸手术中获取了左心室组织样本。我们对线粒体氧化能力、柠檬酸合成酶活性（CSA）、纤维化和淋巴细胞浸润进行了量化。我们认为浸润的 CD3+ 细胞大于 14 个/mm2 即为炎症：结果：ICM 或 DCM 患者在年龄（61.5 ± 5.7 岁对 56.5 ± 12.7 岁，P = 0.164）、性别（86% 对 84%，P = 0.725）、2 型糖尿病（34% 对 18%，P = 0.126）或慢性肾病（8% 对 11%，P = 0.994）方面没有差异。与 DCM 相比，ICM 的氧化能力降低了 23%（108.6 ± 41.4 vs. 141.9 ± 59.9 pmol/（s*mg），P = 0.006）。ICM 和 DCM 的活性氧最大生成量无明显差异（0.59 ± 0.28 vs. 0.69 ± 0.36 pmol/（s*ml），P = 0.196）。通过 CSA 检测线粒体含量，ICM 的线粒体含量较低（359.6 ± 164.1 对 503.0 ± 198.5 nmol/min/mg蛋白，P = 0.002）。值得注意的是，相关炎症在 ICM 中更为常见（27% 对 6%，P = 0.024），浸润白细胞的绝对数量与较低的氧化能力相关（r = -0.296，P = 0.019）。纤维化在 ICM 中更为普遍（占面积的 20.9 ± 21.2 vs. 7.2 ± 5.6%，P = 0.002），但与氧化能力无关（r = -0.13，P = 0.327）：结论：每四名以上患有晚期心房颤动的 ICM 患者中就有一人出现炎症性心肌病范围内的心肌炎症，且与线粒体氧化能力降低有关。未来的研究可能会以标准化的方式评估 ICM 早期阶段的炎症情况，以探索免疫抑制对影响 ICM HF 轨迹的治疗潜力。

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

ESC Heart Failure Medicine-Cardiology and Cardiovascular Medicine

CiteScore

7.00

自引率

7.90%

发文量

461

审稿时长

12 weeks

期刊介绍： ESC Heart Failure is the open access journal of the Heart Failure Association of the European Society of Cardiology dedicated to the advancement of knowledge in the field of heart failure. The journal aims to improve the understanding, prevention, investigation and treatment of heart failure. Molecular and cellular biology, pathology, physiology, electrophysiology, pharmacology, as well as the clinical, social and population sciences all form part of the discipline that is heart failure. Accordingly, submission of manuscripts on basic, translational, clinical and population sciences is invited. Original contributions on nursing, care of the elderly, primary care, health economics and other specialist fields related to heart failure are also welcome, as are case reports that highlight interesting aspects of heart failure care and treatment.