UCP3 调节高脂肪喂养小鼠的心脏效率和线粒体偶联，但不能调节瘦素缺乏小鼠的心脏效率和线粒体偶联。

UCP3 regulates cardiac efficiency and mitochondrial coupling in high fat-fed mice but not in leptin-deficient mice.

机构信息

Division of Endocrinology, Metabolism, and Diabetes and Program in Molecular Medicine, University of Utah School of Medicine, Salt Lake City, Utah, USA.

出版信息

Diabetes. 2012 Dec;61(12):3260-9. doi: 10.2337/db12-0063. Epub 2012 Aug 21.

DOI:10.2337/db12-0063

PMID:22912419

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3501860/

Abstract

These studies investigate the role of uncoupling protein 3 (UCP3) in cardiac energy metabolism, cardiac O(2) consumption (MVO(2)), cardiac efficiency (CE), and mitochondrial uncoupling in high fat (HF)-fed or leptin-deficient mice. UCP3KO and wild-type (WT) mice were fed normal chow or HF diets for 10 weeks. Substrate utilization rates, MVO(2), CE, and mitochondrial uncoupling were measured in perfused working hearts and saponin-permeabilized cardiac fibers, respectively. Similar analyses were performed in hearts of ob/ob mice lacking UCP3 (U3OB mice). HF increased cardiac UCP3 protein. However, fatty acid (FA) oxidation rates were similarly increased by HF diet in WT and UCP3KO mice. By contrast, MVO(2) increased in WT, but not in UCP3KO with HF, leading to increased CE in UCP3KO mice. Consistent with increased CE, mitochondrial coupling was increased in the hearts of HF-fed UCP3KO mice. Unexpectedly, UCP3 deletion in ob/ob mice reduced FA oxidation but had no effect on MVO(2) or CE. In addition, FA-induced mitochondrial uncoupling was similarly enhanced in U3OB compared with ob/ob hearts and was associated with elevated mitochondrial thioesterase-1 protein content. These studies show that although UCP3 may mediate mitochondrial uncoupling and reduced CE after HF feeding, it does not mediate uncoupling in leptin-deficient states.

摘要

这些研究探讨了解偶联蛋白 3（UCP3）在心脏能量代谢、心脏耗氧量（MVO2）、心脏效率（CE）和线粒体解偶联中的作用，分别在高脂肪（HF）喂养或瘦素缺乏的小鼠的心脏中进行。UCP3KO 和野生型（WT）小鼠分别用正常饮食或 HF 饮食喂养 10 周。在灌注工作心脏和皂素通透的心肌纤维中分别测量底物利用速率、MVO2、CE 和线粒体解偶联。在缺乏 UCP3 的 ob/ob 小鼠（U3OB 小鼠）心脏中进行了类似的分析。HF 增加了心脏 UCP3 蛋白。然而，HF 饮食同样增加了 WT 和 UCP3KO 小鼠的脂肪酸（FA）氧化率。相比之下，WT 心脏的 MVO2 增加，但 HF 喂养的 UCP3KO 心脏中没有增加，导致 UCP3KO 小鼠的 CE 增加。与 CE 增加一致，HF 喂养的 UCP3KO 心脏中的线粒体偶联增加。出乎意料的是，ob/ob 小鼠中 UCP3 的缺失减少了 FA 氧化，但对 MVO2 或 CE 没有影响。此外，FA 诱导的线粒体解偶联在 U3OB 心脏中与 ob/ob 心脏相比同样增强，并且与升高的线粒体硫酯酶-1 蛋白含量相关。这些研究表明，尽管 UCP3 可能介导 HF 喂养后的线粒体解偶联和降低的 CE，但它不会介导瘦素缺乏状态下的解偶联。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/add8/3501860/f605d05648ce/3260fig1.jpg

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UCP3 调节高脂肪喂养小鼠的心脏效率和线粒体偶联，但不能调节瘦素缺乏小鼠的心脏效率和线粒体偶联。

UCP3 regulates cardiac efficiency and mitochondrial coupling in high fat-fed mice but not in leptin-deficient mice.

机构信息

Division of Endocrinology, Metabolism, and Diabetes and Program in Molecular Medicine, University of Utah School of Medicine, Salt Lake City, Utah, USA.

出版信息

Diabetes. 2012 Dec;61(12):3260-9. doi: 10.2337/db12-0063. Epub 2012 Aug 21.

DOI:10.2337/db12-0063

PMID:22912419

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3501860/

Abstract

摘要

UCP3 调节高脂肪喂养小鼠的心脏效率和线粒体偶联，但不能调节瘦素缺乏小鼠的心脏效率和线粒体偶联。

UCP3 regulates cardiac efficiency and mitochondrial coupling in high fat-fed mice but not in leptin-deficient mice.

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UCP3 调节高脂肪喂养小鼠的心脏效率和线粒体偶联，但不能调节瘦素缺乏小鼠的心脏效率和线粒体偶联。

UCP3 regulates cardiac efficiency and mitochondrial coupling in high fat-fed mice but not in leptin-deficient mice.

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