在慢性冠心病猪模型中心肌内注射低氧调节细胞外囊泡可增加心肌灌注量

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引用次数: 0

摘要

目的冠状动脉疾病仍然是全球发病率和死亡率的主要原因。晚期冠状动脉疾病患者如果不符合血管内或外科血管再通手术的条件,则选择有限。细胞外囊泡在临床前模型中显示出改善心肌功能的潜力。细胞外囊泡可以通过调节来改变其成分。缺氧条件下的细胞外囊泡已证明能够缩小小动物的心肌梗死面积并减少细胞凋亡。我们的目的是评估低氧调节细胞外囊泡在冠状动脉疾病大型动物模型中的潜在益处。方法通过对左侧环状冠状动脉进行羊膜样收缩,诱导 14 头约克夏猪患冠状动脉疾病。术后两周,猪再次接受左胸廓切开术,注射缺氧调节细胞外囊泡(n = 7)或生理盐水(对照组,n = 7)。结果心肌灌注分析表明,静息时心肌灌注有增加趋势,快速起搏时心肌灌注显著增加(P = .09,P < .001)。与对照组相比,缺氧条件细胞外囊泡组的活化磷酸化内皮一氧化氮合酶、内皮一氧化氮合酶、磷脂酰肌醇 3-激酶、磷酸化蛋白激酶 B 和磷酸化蛋白激酶 B/ 蛋白激酶 B 比率均有明显增加(均为 P <.05)。此外,低氧条件细胞外囊泡组的抗血管生成蛋白胶原 18 和血管抑素显著下降(P = .01, P = .01)。因此,灌注的改善可能是由于一氧化氮信号的改变。低氧调节细胞外囊泡是增加晚期冠心病患者心肌灌注的一种潜在治疗策略。
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Intramyocardial injection of hypoxia-conditioned extracellular vesicles increases myocardial perfusion in a swine model of chronic coronary disease

Objective

Coronary artery disease remains a leading cause of morbidity and mortality worldwide. Patients with advanced coronary artery disease who are not eligible for endovascular or surgical revascularization have limited options. Extracellular vesicles have shown potential to improve myocardial function in preclinical models. Extracellular vesicles can be conditioned to modify their components. Hypoxia-conditioned extracellular vesicles have demonstrated the ability to reduce infarct size and apoptosis in small animals. Our objective is to assess the potential benefits of hypoxia-conditioned extracellular vesicles in a large animal model of coronary artery disease.

Methods

Coronary artery disease was induced in 14 Yorkshire swine by ameroid constriction of the left circumflex coronary artery. Two weeks postsurgery, swine underwent a repeat left thoracotomy for injections of hypoxia-conditioned extracellular vesicles (n = 7) or saline (control, n = 7). Five weeks later, all animals underwent terminal harvest for perfusion measurements and myocardial sectioning.

Results

Myocardial perfusion analysis demonstrated a trend toward increase at rest and a significant increase during rapid pacing (P = .09, P < .001). There were significant increases in activated phosphorylated endothelial nitric oxide synthase, endothelial nitric oxide synthase, phosphatidylinositol 3-kinase, phosphorylated protein kinase B, and the phosphorylated protein kinase B/protein kinase B ratio in the hypoxia-conditioned extracellular vesicles group compared with the control group (all P < .05). Additionally, there was a significant decrease in the antiangiogenic proteins collagen 18 and angiostatin (P = .01, P = .01) in the hypoxia-conditioned extracellular vesicles group.

Conclusions

Intramyocardial injection of hypoxia-conditioned extracellular vesicles results in increased myocardial perfusion without a corresponding change in vessel density. Therefore, this improvement in perfusion is possibly due to changes in nitric oxide signaling. Hypoxia-conditioned extracellular vesicles represent a potential therapeutic strategy to increase myocardial perfusion in patients with advanced coronary artery disease.

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