Akt mitigates ER stress-instigated cardiac dysfunction via regulation of ferroptosis and mitochondrial integrity in a DHODH-dependent manner

IF 5.2 2区医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL

Life sciences Pub Date : 2025-03-29 DOI:10.1016/j.lfs.2025.123591

Na Zhou , Li Ma , Wanting Shi , Russel J. Reiter , Jie Lin , Yingmei Zhang , Dandan Hu , Jun Ren , Kaishou Xu

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引用次数: 0

Abstract

ER stress evokes various types of cell death and myocardial dysfunction. This study aimed to discern the involvement of ferroptosis in chronic Akt activation-offered benefit, if any, against ER stress-triggered cardiac remodeling and contractile anomalies. Cardiac-selective expression of active mutant of Akt (AktOE) and wild-type (WT) mice were challenged with the ER stress instigator tunicamycin (1 mg/kg, 48 h) prior to assessment of cardiac morphology and function. Tunicamycin insult prompted cardiac remodeling (interstitial fibrosis), deranged echocardiographic (higher LVESD, dropped ejection fraction and fractional shortening), cardiomyocyte mechanical and intracellular Ca²⁺ features alongside mitochondrial injury (collapsed mitochondrial membrane potential and ultrastructural change), oxidative stress, compromised Akt-GSK3β signaling, ER stress (upregulated GRP78 and Gadd153), carbonyl formation, apoptosis and ferroptosis (decreased GPX4, SLC7A11). Intriguingly, tunicamycin-evoked anomalies (except GRP78 and Gadd153) were abrogated by Akt activation. Chronic Akt activation negated tunicamycin-induced downregulation of ferric flavin enzyme dihydroorotate dehydrogenase (DHODH), which catalyzes the fourth step of pyrimidine ab initio biosynthesis, and conversion of dihydroorotic acid to orotate. ER stress-induced myocardial anomalies were reversed by the newly identified PI3K activator triptolide, DHODH activator menaquinone-4 and pyrimidine booster coenzyme Q. In vitro experiment revealed that Akt activation- or triptolide-evoked beneficial responses against tunicamycin-induced cardiomyocyte anomalies were cancelled off by DHODH inhibitor BAY2402234 or ferroptosis inducer erastin. These findings support that chronic Akt activation rescues ER stress-evoked myocardial derangements through DHODH-dependent control of ferroptosis and mitochondrial homeostasis.

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Akt通过调控铁下垂和线粒体完整性，以dhodh依赖的方式减轻内质网应激引发的心功能障碍

内质网应激引起各种类型的细胞死亡和心肌功能障碍。本研究旨在发现铁下垂在慢性Akt激活中的作用，如果有的话，对内质网应激引发的心脏重塑和收缩异常有好处。在评估心脏形态和功能之前，用内质网应激刺激剂tunicamycin （1 mg/kg, 48 h）刺激Akt活性突变体（AktOE）和野生型（WT）小鼠的心脏选择性表达。Tunicamycin损伤导致心脏重塑（间质纤维化）、超声心动图紊乱（LVESD升高、射血分数下降和部分缩短）、心肌细胞机械和细胞内Ca2+特征以及线粒体损伤（线粒体膜电位塌陷和超微结构改变）、氧化应激、Akt-GSK3β信号受损、ER应激（GRP78和Gadd153上调）、羰基形成、细胞凋亡和铁凋亡（GPX4、SLC7A11降低）。有趣的是，tunicamycin引起的异常（GRP78和Gadd153除外）被Akt激活消除。慢性Akt激活否定了tunicamycin诱导的铁黄素酶二氢羊角酸脱氢酶（DHODH）的下调，DHODH催化嘧啶从头合成的第四步，并将二氢羊角酸转化为羊角酸。新发现的PI3K激活剂雷公藤甲素、DHODH激活剂甲基萘醌-4和嘧啶增强辅酶q可逆转内质网应激诱导的心肌异常。体外实验表明，Akt激活或雷公藤甲素对tunicamy霉素诱导的心肌细胞异常的有益反应被DHODH抑制剂BAY2402234或铁下垂诱导剂erastin所抵消。这些发现支持慢性Akt激活通过dhodh依赖性控制铁下垂和线粒体稳态来拯救内质网应激引起的心肌紊乱。

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来源期刊

Life sciences 医学-药学

CiteScore

12.20

自引率

1.60%

发文量

841

审稿时长

6 months

期刊介绍： Life Sciences is an international journal publishing articles that emphasize the molecular, cellular, and functional basis of therapy. The journal emphasizes the understanding of mechanism that is relevant to all aspects of human disease and translation to patients. All articles are rigorously reviewed. The Journal favors publication of full-length papers where modern scientific technologies are used to explain molecular, cellular and physiological mechanisms. Articles that merely report observations are rarely accepted. Recommendations from the Declaration of Helsinki or NIH guidelines for care and use of laboratory animals must be adhered to. Articles should be written at a level accessible to readers who are non-specialists in the topic of the article themselves, but who are interested in the research. The Journal welcomes reviews on topics of wide interest to investigators in the life sciences. We particularly encourage submission of brief, focused reviews containing high-quality artwork and require the use of mechanistic summary diagrams.