向心脏输送β-klotho的超声靶向微气泡破坏技术可提高FGF21的敏感性，减轻心肌梗死后的心脏重塑。

IF 5.7 3区医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL

International journal of molecular medicine Pub Date : 2024-04-24 DOI:10.3892/ijmm.2024.5378

Chaofu Yue, RongQin Li, Chunyan Li, Taoxian Yang, Xian Huang, Rong Lei, Yongjun Yan, Yuan Liu, Qiaolin Li, Qinyong Yan, Dingrong Zuo, Shisheng Liu, Mei Yang

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引用次数: 0

摘要

成纤维细胞生长因子（FGF）21是一种能改善线粒体功能和能量代谢的肽类激素，其共同受体β-klotho（KLB）的缺乏会导致FGF21敏感性降低。本研究探讨了通过超声靶向微气泡破坏（UTMD）向心脏输送含有 KLB 基因的质粒是否能增强 FGF21 对急性心肌梗死（AMI）后心力衰竭的疗效。为此，我们使用 ELISA 方法测定了患者和心梗后心功能不全大鼠体内的 FGF21 水平。诱导急性心肌梗死一周后，Sprague-Dawley大鼠接受了3倍UTMD介导的KLB@阳离子微气泡（KLB@CMBs）输送。诱导急性心肌梗死4周后进行超声心动图、组织病理学和生化分析。结果显示，梗塞后心力衰竭患者的血清 FGF21 水平高于健康对照组。然而，在急性心肌梗死大鼠的心脏组织中，下游信号 KLB（而非 α-klotho）降低了。正如预期的那样，使用 FGF21 治疗并不能显著减轻梗死后的心脏重塑。研究发现，心脏中 KLB 受体的减少可能导致对 FGF21 治疗不敏感。在体内，UTMD 技术介导的 KLB@CMBs 向心脏的递送显著增强了 FGF21 对心梗后大鼠心脏重塑和线粒体功能障碍的影响。通过UTMD将KLB输送到心脏并施用FGF21，可通过激活核因子红细胞2相关因子2信号来减轻线粒体损伤和氧化应激。总体而言，本研究表明，向心脏输送 KLB 能显著优化 FGF21 治疗对不良心脏重塑的心脏保护作用。UTMD似乎是一种很有前景的跨学科方法，可用于改善心肌梗死后的心力衰竭。

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Ultrasound‑targeted microbubble destruction technology delivering β‑klotho to the heart enhances FGF21 sensitivity and attenuates heart remodeling post‑myocardial infarction.

Fibroblast growth factor (FGF)21 is a peptide hormone that improves mitochondrial function and energy metabolism, and the deficiency of its co‑receptor β‑klotho (KLB) causes decreased FGF21 sensitivity. The present study examined whether the cardiac delivery of plasmids containing the KLB gene via ultrasound‑targeted microbubble destruction (UTMD) enhances the efficacy of FGF21 against heart failure post‑acute myocardial infarction (AMI). For this purpose, the levels of FGF21 in patients and rats with heart dysfunction post‑infarction were determined using ELISA. Sprague‑Dawley rats received the 3X UTMD‑mediated delivery of KLB@cationic microbubbles (KLB@CMBs) 1 week following the induction of AMI. Echocardiography, histopathology and biochemical analysis were performed at 4 weeks following the induction of AMI. The results revealed that patients with heart failure post‑infarction had higher serum FGF21 levels than the healthy controls. However, the downstream signal, KLB, but not α‑klotho, was reduced in the heart tissues of rats with AMI. As was expected, treatment with FGF21 did not substantially attenuate heart remodeling post‑infarction. It was found that decreased receptors KLB in the heart may result in the insensitivity to FGF21 treatment. In vivo, the UTMD technology‑mediated delivery of KLB@CMBs to the heart significantly enhanced the effects of FGF21 administration on cardiac remodeling and mitochondrial dysfunction in the rats following infarction. The delivery of KLB to the heart by UTMD and the administration of FGF21 attenuated mitochondrial impairment and oxidative stress by activating nuclear factor erythroid 2‑related factor 2 signals. On the whole, the present study demonstrates that the cardiac delivery of KLB significantly optimizes the cardioprotective effects of FGF21 therapy on adverse heart remodeling. UTMD appears a promising interdisciplinary approach with which to improve heart failure post‑myocardial infarction.

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来源期刊

International journal of molecular medicine 医学-医学：研究与实验

CiteScore

12.30

自引率

0.00%

发文量

124

审稿时长

3 months

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