心肌梗死后心力衰竭保留射血分数患者心肌糖酵解代谢产物及其调节蛋白的全景图。
Landscape of glycolytic metabolites and their regulating proteins in myocardium from human heart failure with preserved ejection fraction.
机构信息
Division of Cardiology, Department of Medicine, Johns Hopkins University School of Medicine, Baltimore, MD, USA.
Department of Chemistry and Molecular Biology, Johns Hopkins Bloomberg School of Public Health, and Department of Oncology, Johns Hopkins University School of Medicine, Baltimore, MD, USA.
出版信息
Eur J Heart Fail. 2024 Sep;26(9):1941-1951. doi: 10.1002/ejhf.3389. Epub 2024 Aug 9.
AIMS
Heart failure (HF) with preserved ejection fraction (HFpEF) reflects half of all clinical HF yet has few therapies. Obesity and diabetes are now common comorbidities which have focused attention towards underlying myocardial metabolic defects. The profile of a major metabolic pathway, glycolytic intermediates and their regulating enzymes and ancillary pathways, remains unknown.
METHODS AND RESULTS
Endomyocardial biopsies from HFpEF (n = 37) and non-failing controls (n = 21) were assayed by non-targeted or targeted metabolomics and immunoblot to determine glycolytic and ancillary pathway metabolites and protein expression of their regulating enzymes. Glucose and GLUT1 expression were higher in HFpEF, but prominent glycolytic metabolites: glucose-6-phosphate, fructose-1,6-biphosphate (F1,6bP), and 3-phosphoglycerate were reduced by -78%, -91%, and -73%, respectively, versus controls. Expression of their corresponding synthesizing enzymes hexokinase, phospho-fructokinase, and phosphoglycerate kinase were also significantly lower (all p < 0.0005). Pentose phosphate and hexosamine biosynthetic pathway metabolites were reduced while glycogen content increased. Despite proximal reduction in key glycolytic intermediates, pyruvate increased but mitochondrial pyruvate transporter (MPC1) expression was reduced. Pyruvate dehydrogenase converting pyruvate to acetyl-CoA was more activated but some Krebs cycle intermediates were reduced. This HFpEF glycolytic profile persisted after adjusting for body mass index (BMI), diabetes, age, and sex, or in subgroup analysis with controls and HFpEF matched for BMI and diabetes/insulin history. In HFpEF, BMI but not glycated haemoglobin negatively correlated with F1,6bP (p = 7e-5, r = -0.61) and phosphoenolpyruvate (p = 0.006, r = -0.46).
CONCLUSIONS
Human HFpEF myocardium exhibits reduced glycolytic and ancillary pathway intermediates and expression of their synthesizing proteins. This combines features reported in HF with reduced ejection fraction and obesity/diabetes that likely exacerbate metabolic inflexibility.
目的
射血分数保留型心力衰竭(HFpEF)反映了所有临床心力衰竭的一半,但治疗方法很少。肥胖症和糖尿病现在是常见的合并症,这引起了人们对潜在心肌代谢缺陷的关注。主要代谢途径、糖酵解中间产物及其调节酶和辅助途径的特征仍不清楚。
方法和结果
通过非靶向或靶向代谢组学和免疫印迹分析,测定 HFpEF(n=37)和非衰竭对照组(n=21)的心内膜心肌活检,以确定糖酵解和辅助途径代谢物以及调节酶的蛋白表达。HFpEF 中的葡萄糖和 GLUT1 表达较高,但显著的糖酵解代谢物:葡萄糖-6-磷酸、果糖-1,6-二磷酸(F1,6bP)和 3-磷酸甘油酸分别减少了 -78%、-91%和-73%,与对照组相比。其相应合成酶己糖激酶、磷酸果糖激酶和磷酸甘油酸激酶的表达也显著降低(均 p<0.0005)。戊糖磷酸和己糖胺生物合成途径的代谢物减少,而糖原含量增加。尽管关键糖酵解中间产物的近端减少,但丙酮酸增加,但线粒体丙酮酸转运体(MPC1)的表达减少。丙酮酸脱氢酶将丙酮酸转化为乙酰辅酶 A 的活性更高,但一些三羧酸循环中间产物减少。HFpEF 的这种糖酵解特征在调整体重指数(BMI)、糖尿病、年龄和性别后仍然存在,或者在与 BMI 匹配的对照组和 HFpEF 亚组分析中,以及与糖尿病/胰岛素史匹配的 HFpEF 亚组分析中仍然存在。在 HFpEF 中,BMI 而不是糖化血红蛋白与 F1,6bP(p=7e-5,r=-0.61)和磷酸烯醇丙酮酸(p=0.006,r=-0.46)呈负相关。
结论
人类 HFpEF 心肌表现出糖酵解和辅助途径中间产物以及合成蛋白表达减少。这结合了射血分数降低型心力衰竭和肥胖/糖尿病中报道的特征,这些特征可能会加剧代谢灵活性下降。
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