Ma Kaiyue, Sun Lu, Jia Chunxue, Kui Hongqian, Xie Jiaqi, Zang Shidan, Huang Shixin, Que Jinfeng, Liu Chuanxin, Huang Jianmei
School of Chinese Materia Medica, Beijing University of Chinese Medicine, Beijing, China.
College of Chinese Materia Medica and Food Engineering, Shanxi University of Chinese Medicine, Jinzhong, China.
Front Pharmacol. 2024 Sep 24;15:1378758. doi: 10.3389/fphar.2024.1378758. eCollection 2024.
Podophyllotoxin (PPT) is a high-content and high-activity compound extracted from the traditional Chinese medicinal plant () which exhibits various biological activities. However, its severe toxicity limits its use. In clinical settings, patients with poisoning often experience adverse reactions when taking large doses in a short period. The heart is an important toxic target organ, so it is necessary to conduct 24-h acute cardiac toxicity studies on PPT to understand its underlying toxicity mechanism.
Based on the concept of the toxicological evidence chain (TEC), we utilized targeted metabolomic and transcriptomic analyses to reveal the mechanism of the acute cardiotoxicity of PPT. The manifestation of toxicity in Sprague-Dawley rats, including changes in weight and behavior, served as Injury Phenotype Evidence (IPE). To determine Adverse Outcomes Evidence (AOE), the hearts of the rats were evaluated through histopathological examination and by measuring myocardial enzyme and cardiac injury markers levels. Additionally, transcriptome analysis, metabolome analysis, myocardial enzymes, and cardiac injury markers were integrated to obtain Toxic Event Evidence (TEE) using correlation analysis.
The experiment showed significant epistaxis, hypokinesia, and hunched posture in PPT group rats within 24 h after exposure to 120 mg/kg PPT. It is found that PPT induced cardiac injury in rats within 24 h, as evidenced by increased serum myocardial enzyme levels, elevated concentrations of cardiac injury biomarkers, and altered cardiac cell morphology, all indicating some degree of cardiac toxicity. Transcriptome analysis revealed that primary altered metabolic pathway was arachidonic acid metabolism after PPT exposure. Cyp2e1, Aldob were positively correlated with differential metabolites, while DHA showed positive correlation with differential genes Fmo2 and Timd2, as well as with heart injury markers BNP and Mb.
This study comprehensively evaluated cardiac toxicity of PPT and initially revealed the mechanism of PPT-induced acute cardiotoxicity, which involved oxidative stress, apoptosis, inflammatory response, and energy metabolism disorder.
鬼臼毒素(PPT)是从传统中药植物(此处原文缺失植物名称)中提取的一种高含量、高活性的化合物,具有多种生物活性。然而,其严重的毒性限制了其应用。在临床环境中,鬼臼毒素中毒的患者在短时间内大剂量服用时经常会出现不良反应。心脏是一个重要的毒性靶器官,因此有必要对鬼臼毒素进行24小时急性心脏毒性研究,以了解其潜在的毒性机制。
基于毒理学证据链(TEC)的概念,我们利用靶向代谢组学和转录组学分析来揭示鬼臼毒素急性心脏毒性的机制。Sprague-Dawley大鼠的毒性表现,包括体重和行为的变化,作为损伤表型证据(IPE)。为了确定不良结局证据(AOE),通过组织病理学检查以及测量心肌酶和心脏损伤标志物水平来评估大鼠的心脏。此外,通过相关性分析将转录组分析、代谢组分析、心肌酶和心脏损伤标志物整合起来,以获得毒性事件证据(TEE)。
实验表明,暴露于120mg/kg鬼臼毒素后24小时内,PPT组大鼠出现明显的鼻出血、运动减退和弓背姿势。研究发现,鬼臼毒素在24小时内诱导大鼠心脏损伤,血清心肌酶水平升高、心脏损伤生物标志物浓度升高以及心脏细胞形态改变均证明了这一点,所有这些都表明存在一定程度的心脏毒性。转录组分析显示,鬼臼毒素暴露后主要改变的代谢途径是花生四烯酸代谢。Cyp2e1、Aldob与差异代谢物呈正相关,而DHA与差异基因Fmo2和Timd2以及心脏损伤标志物BNP和Mb呈正相关。
本研究全面评估了鬼臼毒素的心脏毒性,并初步揭示了鬼臼毒素诱导急性心脏毒性的机制,该机制涉及氧化应激、细胞凋亡、炎症反应和能量代谢紊乱。
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