心肌自噬缺陷可减弱心钠肽的产生并破坏心肌-脂肪细胞的相互作用，导致脂肪蓄积增加和代谢功能障碍。

Cardiac Autophagy Deficiency Attenuates ANP Production and Disrupts Myocardial-Adipose Cross Talk, Leading to Increased Fat Accumulation and Metabolic Dysfunction.

机构信息

Department of Biology, York University, Toronto, Canada.

The First Affiliated Hospital, Jinan University, Guangzhou, China.

出版信息

Diabetes. 2021 Jan;70(1):51-61. doi: 10.2337/db19-0762. Epub 2020 Oct 12.

DOI:10.2337/db19-0762

PMID:33046483

Abstract

Increased myocardial autophagy has been established as an important stress-induced cardioprotective response. Three weeks after generating cardiomyocyte-specific autophagy deficiency, via inducible deletion of autophagy-related protein 7 (Atg7), we found that these mice (AKO) had increased body weight and fat mass without altered food intake. Glucose and insulin tolerance tests indicated reduced insulin sensitivity in AKO mice. Metabolic cage analysis showed reduced ambulatory activity and oxygen consumption with a trend of elevated respiratory exchange ratio in AKO mice. Direct analysis of metabolism in subcutaneous and visceral adipocytes showed increased glucose oxidation and reduced ATGL expression and HSL phosphorylation with no change in lipid synthesis or fatty acid oxidation. Importantly, we found AKO mice had reduced myocardial and circulating levels of atrial natriuretic peptide (ANP), an established mediator of myocardial-adipose cross talk. When normal ANP levels were restored to AKO mice with use of osmotic pump, the metabolic dysfunction evident in AKO mice was corrected. We conclude that cardiac autophagy deficiency alters myocardial-adipose cross talk via decreased ANP levels with adverse metabolic consequences.

摘要

心肌自噬增加已被确定为一种重要的应激诱导性心脏保护反应。通过诱导性敲除自噬相关蛋白 7（Atg7），在产生心肌细胞特异性自噬缺乏症 3 周后，我们发现这些小鼠（AKO）体重和脂肪量增加，而食物摄入量没有改变。葡萄糖和胰岛素耐量试验表明 AKO 小鼠的胰岛素敏感性降低。代谢笼分析显示 AKO 小鼠的活动量和耗氧量减少，呼吸交换率有升高趋势。对皮下和内脏脂肪细胞的代谢直接分析显示，葡萄糖氧化增加，脂肪酶表达和激素敏感脂肪酶磷酸化减少，而脂质合成或脂肪酸氧化没有变化。重要的是，我们发现 AKO 小鼠的心肌和循环心房利钠肽（ANP）水平降低，而 ANP 是心肌-脂肪相互作用的一种已确立的介质。当使用渗透泵将正常的 ANP 水平恢复到 AKO 小鼠时，AKO 小鼠明显的代谢功能障碍得到纠正。我们的结论是，心脏自噬缺乏通过降低 ANP 水平改变心肌-脂肪相互作用，从而产生不良的代谢后果。

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心肌自噬缺陷可减弱心钠肽的产生并破坏心肌-脂肪细胞的相互作用，导致脂肪蓄积增加和代谢功能障碍。

Cardiac Autophagy Deficiency Attenuates ANP Production and Disrupts Myocardial-Adipose Cross Talk, Leading to Increased Fat Accumulation and Metabolic Dysfunction.

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