用磷酸二酯酶2A进行心脏基因治疗可限制心力衰竭小鼠模型中的重塑和心律失常。
Cardiac Gene Therapy With Phosphodiesterase 2A Limits Remodeling and Arrhythmias in Mouse Models of Heart Failure.
作者信息
Kamel Rima, Bourcier Aurélia, Margaria Jean Piero, Jin Valentin, Varin Audrey, Hivonnait Agnès, Mercier-Nomé Françoise, Mika Delphine, Ghigo Alessandra, Charpentier Flavien, Algalarrondo Vincent, Hirsch Emilio, Fischmeister Rodolphe, Vandecasteele Grégoire, Leroy Jérôme
机构信息
Université Paris-Saclay, Inserm, Signaling and Cardiovascular Pathophysiology, UMR-S 1180 Orsay France.
Molecular Biotechnology Center "Guido Tarone", Department of Molecular Biotechnology and Health Sciences University of Torino Italy.
出版信息
J Am Heart Assoc. 2025 Feb 4;14(3):e037343. doi: 10.1161/JAHA.124.037343. Epub 2025 Feb 3.
BACKGROUND
PDE2 (phosphodiesterase 2) is upregulated in human heart failure. Cardiac PDE2-transgenic mice are protected against contractile dysfunction and arrhythmias in heart failure but whether an acute elevation of PDE2 could be of therapeutic value remains elusive. This hypothesis was tested using cardiac PDE2 gene transfer in preclinical models of heart failure.
METHODS AND RESULTS
C57BL/6 male mice were injected with serotype 9 adeno-associated viruses encoding for PDE2A. This led to a ≈10-fold rise of PDE2A protein levels that affected neither cardiac structure nor function in healthy mice. Two weeks after inoculation with serotype 9 adeno-associated viruses, mice were implanted with minipumps delivering either NaCl, isoproterenol (60 mg/kg per day), or isoproterenol and phenylephrine (30 mg/kg per day each) for 2 weeks. In mice injected with serotype 9 adeno-associated viruses encoding for LUC (luciferase), isoproterenol or isoproterenol+phenylephrine infusion induced left ventricular hypertrophy, decreased ejection fraction unveiled by echocardiography, and promoted fibrosis and apoptosis assessed by Masson's trichrome and Tunel, respectively. Furthermore, inotropic responses to isoproterenol of ventricular cardiomyocytes isolated from isoproterenol+phenylephrine-LUC mice loaded with 1 μmol/L Fura-2AM and stimulated at 1 Hz to record calcium transients and sarcomere shortening were dampened. Spontaneous calcium waves at the cellular level were promoted as well as ventricular arrhythmias evoked in vivo by catheter-mediated ventricular pacing after isoproterenol (1.5 mg/kg) and atropine (1 mg/kg) injection. However, increased PDE2A blunted these adverse outcomes evoked by sympathomimetic amines.
CONCLUSIONS
Cardiac gene therapy with PDE2A limits left ventricle remodeling, dysfunction, and arrhythmias evoked by catecholamines, providing evidence that increasing PDE2A activity acutely could prevent progression toward heart failure.
背景
磷酸二酯酶2(PDE2)在人类心力衰竭中上调。心脏PDE2转基因小鼠可免受心力衰竭时的收缩功能障碍和心律失常影响,但PDE2急性升高是否具有治疗价值仍不清楚。本研究在心力衰竭临床前模型中通过心脏PDE2基因转移对这一假说进行了验证。
方法与结果
给C57BL/6雄性小鼠注射编码PDE2A的9型腺相关病毒。这导致PDE2A蛋白水平升高约10倍,且对健康小鼠的心脏结构和功能均无影响。接种9型腺相关病毒两周后,给小鼠植入微型泵,持续2周输注氯化钠、异丙肾上腺素(每天60mg/kg)或异丙肾上腺素和去氧肾上腺素(各每天30mg/kg)。在注射编码荧光素酶(LUC)的9型腺相关病毒的小鼠中,输注异丙肾上腺素或异丙肾上腺素+去氧肾上腺素可诱导左心室肥厚,超声心动图显示射血分数降低,并分别通过Masson三色染色和Tunel法评估促进纤维化和细胞凋亡。此外,从加载1μmol/L Fura-2AM并以1Hz刺激以记录钙瞬变和肌节缩短的异丙肾上腺素+去氧肾上腺素-LUC小鼠分离的心室心肌细胞,对异丙肾上腺素的变力反应减弱。细胞水平的自发钙波增加,异丙肾上腺素(1.5mg/kg)和阿托品(1mg/kg)注射后,通过导管介导的心室起搏在体内诱发的室性心律失常也增加。然而,PDE2A增加可减轻拟交感胺引起的这些不良后果。
结论
PDE2A心脏基因治疗可限制儿茶酚胺引起的左心室重构、功能障碍和心律失常,这表明急性增加PDE2A活性可预防心力衰竭进展。
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