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Metabolic syndrome and chronic simvastatin therapy enhanced human cardiomyocyte stress before and after ischemia-reperfusion in cardio-pulmonary bypass patients

机译:代谢综合征和辛伐他汀慢性疗法可增强体外循环患者缺血再灌注前后的心肌细胞应激

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Metabolic syndrome (MetS) is a set of metabolic alterations including high levels of low-density lipoprotein (LDL), which increase the risk of cardiomyopathy often leading to surgery. Despite inducing myopathy, statins are widely used to lower LDL. Cardiopulmonary bypass (Cpb) causes oxidative stress and metabolic injury, altering mitochondrial expression (Grp75) and endoplasmic reticulum (Grp78) chaperones, apoptotic enzymes (Bcl2 family) and increasing cardiomyocyte lipid/lipofuscin storage. We believe that cardiomyocytes from patients with MetS may be more sensitive to surgical stress, in particular after simvastatin therapy (MetS+Stat). The study group included ten patients with MetS, ten patients with Mets+Stat and ten healthy subjects. Myocardial biopsies were obtained both before and after-Cpb. Grp75, Grp78, Bax, Bcl2, lipids, lipofuscin and fibrosis were evaluated by immuno/histochemistry. MetS cardiomyocytes had higher Grp75, Bax, fibrosis and lipofuscin. MetS+Stat had lower Grp75 and higher Grp78 expressions, high Bax, fewer fibrosis and higher lipofuscin content. Cpb did not vary the fibrosis and lipids/lipofuscin content, although it influenced the chaperones and Bax expression in all groups. These changes were more profound in patients with MetS and even more so in patients with MetS+Stat. The results suggest that MetS and MetS+Stat cardiomyocytes were more highly stressed after-Cpb. Interestingly, simvastatin caused high stress even before-Cpb.
机译:代谢综合征(MetS)是一组代谢改变,包括高水平的低密度脂蛋白(LDL),这会增加经常导致手术的心肌病风险。尽管诱发肌病,他汀类药物仍被广泛用于降低LDL。体外循环(Cpb)会引起氧化应激和代谢损伤,从而改变线粒体表达(Grp75)和内质网(Grp78)伴侣,凋亡酶(Bcl2家族)并增加心肌细胞脂质/脂褐素的储存。我们认为,患有MetS的患者的心肌细胞可能对手术压力更为敏感,尤其是在辛伐他汀治疗后(MetS + Stat)。研究组包括十名MetS患者,十名Mets + Stat患者和十名健康受试者。在Cpb之前和之后都进行了心肌活检。通过免疫/组织化学评估Grp75,Grp78,Bax,Bcl2,脂质,脂褐素和纤维化。 MetS心肌细胞具有较高的Grp75,Bax,纤维化和脂褐素。 MetS + Stat具有较低的Grp75和较高的Grp78表达,较高的Bax,较少的纤维化和较高的脂褐素含量。尽管Cpb影响所有组中的伴侣蛋白和Bax表达,但其纤维化和脂质/脂褐素含量均无变化。这些变化在MetS患者中更为深刻,在MetS + Stat患者中更为明显。结果表明,Cpb后MetS和MetS + Stat心肌细胞的压力更高。有趣的是,辛伐他汀甚至在Cpb之前就引起了高压力。

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